TIDMHCM
RNS Number : 1547H
Hutchison China Meditech Limited
30 July 2019
Chi-Med Reports 2019 Interim Results and Provides Updates on
Key Clinical Programs
London: Tuesday, July 30, 2019: Hutchison China MediTech Limited
("Chi-Med") (AIM/Nasdaq: HCM) today announces its unaudited
financial results for the six months ended June 30, 2019 and
provides updates on key clinical programs. Major highlights
include:
-- Positive surufatinib China Phase III study in non-pancreatic neuroendocrine tumors ("NET")
- Interim analysis of SANET-ep study confirmed to have met primary endpoint and the Independent
Data Monitoring Committee ("IDMC") recommended the study be un-blinded, a year ahead of schedule.
New Drug Application ("NDA") is now being prepared for submission during 2019;
-- Early progress on Elunate(R) (fruquintinib capsules) with China in-market sales in colorectal
cancer ("CRC") of $11.4 million1 (RMB77.1 million) during H1 2019; Discussions in progress
for potential inclusion in the China National Reimbursement Drug List ("NRDL") at the next
update in Q4 2019;
-- Potential for first savolitinib NDA targeted for H1 2020 - for MET2 Exon 14 deletion non-small
cell lung cancer ("NSCLC") in China. Oral presentations of savolitinib data made at scientific
conferences in H1 2019 in lung cancer (monotherapy and combination with Tagrisso(R)) and kidney
cancer (combination with Imfinzi(R)).
Video webcast presentation at 9:00 a.m. BST and additional
conference call at 9:00 a.m. EDT.
"Chi-Med's business is progressing well on all fronts." said
Simon To, Chairman, Chi-Med. "All major clinical readouts in the
first half were encouraging, with the stand-out results being
surufatinib's positive Phase III outcome in non-pancreatic NET and
savolitinib's preliminary data in MET Exon 14 deletion NSCLC along
with the completion of enrollment of its registration study. We
believe these accomplishments have the potential to support
Chi-Med's next two NDA submissions, surufatinib later this year and
savolitinib early next year."
"Highly encouraging preliminary data was also reported for the
savolitinib / Tagrisso(R) combination in NSCLC, which led to the
initiation of a global registration intent trial by AstraZeneca AB
(publ) ("AstraZeneca"), the SAVANNAH study, early this year. Also,
recently released preliminary data for the savolitinib / Imfinzi(R)
combination in kidney cancer is promising."
"Our first approved oncology drug, Elunate(R) , is making
progress, with first six-month revenue well ahead, at the same
stage, of the five small molecule VEGFR(3) inhibitors previously
launched by multinational companies in China. In our view, with
time and inclusion in the China NRDL, Elunate(R)' s well documented
efficacy and safety profile will make it a formidable
competitor."
"Business is as usual for our Commercial Platform, which
generated 9% net income growth on a CER(4) basis versus same period
last year. This income helps significantly to fund our clinical
development programs as well as our discovery engine which produced
yet another exciting oncology asset, our ninth, with the IND(5)
submission of our novel IDH 1/2 inhibitor(6) HMPL-306."
"Our organization is expanding rapidly, with our New
Jersey-based international clinical and regulatory team scaling up
to manage global registration studies on surufatinib and
fruquintinib and early development on our B-cell malignancy assets.
Our in-house oncology commercial team in China is also growing
fast, managing medical affairs and getting ready for the potential
launch of surufatinib late next year."
"Looking ahead at the next two years, we expect to accelerate
our transformation into a fully integrated and globally-facing
biopharmaceutical company with capability to discover, develop and
launch multiple novel drug innovations aimed at addressing a broad
range of unmet medical needs and benefiting a large number of
patients."
Financial Highlights
The items below are selected financial data for the six months
ended June 30, 2019. All monetary figures are expressed in U.S.
dollars unless otherwise stated. For more details, please refer to
"Financial Review", "Operations Review" and "Interim Unaudited
Condensed Consolidated Financial Statements" below.
OVERALL GROUP: sufficient resources to reach multiple value
inflection points on our pipeline
-- Group revenue $102.2 million (H1-18: $102.2m).
-- Net loss attributable to Chi--Med of $45.4 million (H1-18: net loss of $32.7m).
-- Adjusted Group net cash flows (non-GAAP) was -$63.7 million in H1 2019 including the repayment
of a total of $26.9 million in bank loans, leaving the Group with no outstanding bank borrowings.
Cash from our Commercial Platform, as well as payments received from our multinational partners,
continued to offset a material part of our research and development ("R&D") expenses.
-- Cash resources of $383.6 million at Group level as of June 30, 2019 (December 31, 2018: $420.3m),
including cash, cash equivalents and short-term investments of $237.3 million (December 31,
2018: $301.0m) and unutilized bank facilities of $146.3 million (December 31, 2018: $119.3m).
INNOVATION PLATFORM: increased investment in R&D driven by
expansion of our organization, operations and progress on our
clinical development pipeline
-- Consolidated revenue was $12.0 million (H1-18: $13.6m) mainly due to payments from AstraZeneca
and Lilly. During H1 2019, following the launch of Elunate(R) in late 2018, we recorded $5.5
million (H1-18: $1.1m) in manufacturing and service fee revenues as well as royalty income
from Lilly.
-- R&D expenses on an as adjusted (non-GAAP) basis increased to $74.5 million (H1-18: $66.7m),
primarily driven by the progress in the development of our eight clinical drug candidates,
five of which are either in or about to start development outside China; the ramp-up of our
small molecule manufacturing operations in Suzhou; expansion of U.S. and international clinical
and regulatory operations; and establishment of our oncology commercial infrastructure in
China.
-- Net loss from our Innovation Platform attributable to Chi-Med of $63.8 million (H1-18: net
loss of $52.9m).
COMMERCIAL PLATFORM: solid net income growth on a CER basis due
to continued progress in our Prescription Drugs business
-- Total consolidated sales grew 2% (7% at CER) to $90.2 million (H1-18: $88.6m) mainly due to
progress on our Prescription Drugs subsidiary Hutchison Sinopharm(7) being partially offset
by rationalization of certain low contribution products in the Consumer Health business.
-- Total sales of non-consolidated joint ventures increased 2% (8% at CER) to $276.9 million
(H1-18: $271.7m) driven by solid performance on our leading prescription cardiovascular drug,
She Xiang Bao Xin ("SXBX") pill, which grew 9% (15% at CER) to $141.0 million (H1-18: $129.8m).
-- Total consolidated net income from our Commercial Platform attributable to Chi-Med increased
3% (9% at CER) to $27.7 million (H1-18: $26.9m).
---
U.K. Analysts Meeting and Webcast Scheduled Today at 9:00 a.m.
BST (4:00 p.m. HKT) - at Citigate Dewe Rogerson, 8th Floor, Holborn
Gate, 26 Southampton Buildings, London WC2A 1AN, UK. Investors may
participate in the call at +44 20 3003 2666 (800 900 476 toll free
in Hong Kong), or access a live video webcast of the call via
Chi-Med's website at
www.chi-med.com/investors/event-information/.
U.S. Conference Call Scheduled Today at 9:00 a.m. EDT - to
participate in the call from the U.S., please dial 1 866 966
5335.
Additional dial-in numbers are also available at Chi-Med's
website. For both calls please use conference ID "Chi-Med."
([1]) In-market sales figures for Elunate(R) are based on
information provided by Eli Lilly and Company ("Lilly");
([2]) mesenchymal epithelial transition receptor ("MET");
([3]) Vascular endothelial growth factor receptor ("VEGFR");
([4]) Constant Exchange Rate ("CER"). Certain financial
information in this announcement is presented on a constant
exchange rate basis, or at CER. These financial measures are not
prepared in accordance with U.S. generally accepted accounting
principles (GAAP) because they remove the effects of currency
movements from our reported results. Please refer to "Use of
Non-GAAP Financial Measures and Reconciliation" below for further
information relevant to the interpretation of these financial
measures and reconciliations of these financial measures to the
most comparable GAAP measures;
([5]) Investigational New Drug ("IND");
([6]) Isocitrate dehydrogenase ("IDH") 1 and 2;
([7]) Hutchison Whampoa Sinopharm Pharmaceuticals (Shanghai)
Company Limited ("Hutchison Sinopharm").
Operating HIGHLIGHTS
The points below summarize some of Chi-Med's operating
highlights so far this year. For more details, please refer to
"Operations Review" below.
SURUFATINIB (HMPL-012 or sulfatinib) - angio-immuno kinase
inhibitor of VEGFR 1/2/3, fibroblast growth factor receptor
("FGFR") 1, and colony stimulating factor-1 receptor
("CSF-1R"):
-- Positive China Phase III in non-pancreatic NET: An interim analysis in June 2019 confirmed
that the Phase III non-pancreatic NET (SANET-ep) study met its primary endpoint of progression-free
survival ("PFS"). As a result, the IDMC recommended the study be un-blinded, a year ahead
of schedule, and preparations are now underway for an NDA submission in late 2019 for this
indication in China;
-- Initiated China Phase II/III in biliary tract cancer ("BTC"): Based on preliminary Phase Ib/IIa
data, we initiated a Phase IIb/III registration study in BTC in China in March 2019; and
-- Initiated PD-1 combination development: Received China IND clearance during early 2019 and
initiated a Phase I safety run-in study in China of surufatinib plus Tuoyi(R) , an approved
PD-1 monoclonal antibody from Shanghai Junshi Biosciences Co. Ltd. ("Junshi").
FRUQUINTINIB - highly selective tyrosine kinase inhibitor
("TKI") of VEGFR 1/2/3 - potential best-in-class in terms of both
efficacy and safety:
-- Early progress on Elunate(R) (fruquintinib capsules) in third-line CRC in China:
o $11.4 million (RMB77.1 million) in sales during H1 2019: In-market sales of Elunate(R) to
third-parties, as provided by Lilly, in the first full six-month period since its November
25, 2018 launch;
o Progress in reimbursement discussion: Elunate(R) was included in the Shanghai provincial reimbursement
drug list ("RDL") in June 2019. Discussions now in-progress for potential inclusion in the
China NRDL at the next update in early Q4 2019.
-- Cleared Phase III interim analysis in second-line gastric cancer: In April 2019, we conducted
an interim analysis of the FRUTIGA study in China for futility. The analysis evaluated PFS
and overall survival ("OS") trends after six months of therapy for the first 100 patients
in the study. The IDMC recommended to continue the study without changes; and
-- Initiated PD-1 combination development: Received China IND clearance in early 2019 and initiated
a Phase I study of fruquintinib plus Tyvyt(R) , an approved PD-1 monoclonal antibody from
Innovent Biologics (Suzhou) Co. Ltd. ("Innovent"). Phase I development of fruquintinib plus
genolimzumab, a PD-1 monoclonal antibody under development by Genor Biopharma Co. Ltd. ("Genor")
is also now underway.
SAVOLITINIB - potential first-in-class selective MET inhibitor
in late-stage clinical development:
-- Reached enrollment goal in Phase II registration study - MET Exon 14 deletion NSCLC: Encouraging
interim data, for 31 evaluable patients, for the China Phase II registration study in MET
Exon 14 deletion NSCLC were presented during the 2019 American Association for Cancer Research
("AACR") Annual Meeting. We have now reached our enrollment goal for this Phase II registration
study, and subject to clinical outcome, with potential to be our first NDA submission for
savolitinib in early 2020;
-- AstraZeneca collaboration, leading global position in EGFR-TKI resistant NSCLC:
o 56% objective response rate ("ORR") and 7.1 months' median duration of response - in patients
with acquired resistance to Iressa(R) or Tarceva(R) driven by MET amplification: Preliminary
TATTON Phase Ib/IIa data for the savolitinib/Tagrisso(R) combination regimen were presented
at the 2019 AACR Annual Meeting for a total of 43 evaluable patients who were T790M- and had
not previously received a third-generation EGFR inhibitor;
o 31% ORR and 9.7 months' median duration of response - in patients with acquired resistance
to Tagrisso(R) driven by MET amplification: Preliminary TATTON Phase Ib/IIa data for the
savolitinib/Tagrisso(R)
combination regimen were also presented at the 2019 AACR Annual Meeting for a total of 39
evaluable patients who had reported disease progression after receiving a third-generation
EGFR inhibitor. The SAVANNAH Phase IIb registration intent study, which is being conducted
in North and South America, Europe and Asia in this target patient population, dosed its first
patient in early 2019;
-- Emerging signal for savolitinib/Imfinzi(R) (PD-L1) combination in renal cell carcinoma ("RCC"):
Interim results for the papillary RCC ("PRCC") cohort of the CALYPSO Phase II study were presented
at the 2019 American Society of Clinical Oncology Genitourinary Symposium ("ASCO GU") reporting
a 27% ORR for all 41 patients and a 32% ORR for the 28 previously untreated patients. The
combination was tolerable and associated with durable responses in PRCC.
Further progress in early/proof-of-concept clinical trials and
discovery, including:
-- HMPL-523 - potential first-in-class selective Syk inhibitor: A Phase Ib dose expansion study
in both China and Australia accelerated enrollment in H1 2019 in multiple sub-types of non-Hodgkin's
lymphoma ("NHL"). We intend to use Phase Ib data to guide registration strategy in China during
late 2019; and multiple U.S. / Europe sites are also now open for a Phase I/Ib study with
patient screening underway.
-- HMPL-689 - potential best-in-class selective PI3K inhibitor: A recommended dose for Phase
II study has been selected based on the China Phase I study; U.S. / Europe IND applications
cleared; and
-- IND submission in China for HMPL-306: A novel selective small molecule TKI of isocitrate dehydrogenase
("IDH") 1/2, discovered in-house with IND submitted H1 2019.
Major organizational expansion, including:
-- Expansion of international clinical and regulatory operations: accelerated expansion of New
Jersey team to support development of multiple un-partnered compounds outside of Asia; and
-- Establishment of China oncology commercial organization: currently numbering about 60 commercial
staff, primarily focused on medical affairs and preparation for potential surufatinib launch
in late 2020.
POTENTIAL UPCOMING KEY EVENTS
China - H2 2019 Global - H2 2019
---------------------------------------- ---------------------------------------
1. Savolitinib - Registration study 1. HMPL-523 (Syk) - Phase I - Initiate
completion - MET Exon 14 deletion U.S. / E.U. Phase I/Ib in indolent
NSCLC (occurred July); NHL;
2. Surufatinib - Phase III data 2. HMPL-689 (PI3K ) - Phase I -
(SANET-ep) -presentation at scientific Initiate U.S. / E.U. Phase I/Ib
conference; in indolent NHL;
3. Surufatinib - NDA submission 3. Savolitinib - Phase II data
- in non-pancreatic NET; (VIKTORY) - gastric cancer data
(patient tumor molecular profiling).
4. Fruquintinib - Phase III data
(FALUCA) - submit for presentation
in NSCLC at conference;
5. Fruquintinib - Reimbursement
- possible Elunate(R) inclusion
in China NRDL in Q4 2019.
China - H1 2020 Global - H1 2020
------------------------------------ ---------------------------------------
6. Fruquintinib - Phase III interim 4. Surufatinib - Phase II/III start
analysis (FRUTIGA) - 2(nd) interim - initiate U.S. / E.U. study in
in gastric cancer; pancreatic NET;
7. Surufatinib - Phase III interim 5. Fruquintinib - Phase II/III
analysis (SANET-p) - planned final start - initiate U.S. / E.U. Phase
interim analysis; II/III study in metastatic CRC;
8. Savolitinib - NDA submission 6. Savolitinib - Phase II data
- in MET Exon 14 deletion NSCLC; (CALYPSO) - Imfinzi(R) (PD-L1)
combo in RCC;
9. Surufatinib - Phase Ib/II data 7. Savolitinib - Phase II registration
- submit for presentation of BTC study (SAVANNAH) interim analysis
at conference; - in NSCLC;
10. HMPL-523 - Phase II study start
- potential registration study
indolent NHL.
FINANCIAL GUIDANCE
We are providing the following updated Financial Guidance for
the year ending December 31, 2019. Our updated guidance takes into
account the weakening of the RMB, which was down 6% against the
U.S. dollar during H1 2019 (using the average exchange rate for the
period) relative to the same period last year due to global
macroeconomic factors. We expect this trend to continue through the
balance of 2019, and this depreciation of the RMB has the effect of
reducing our R&D expenses in China in U.S. dollar terms.
In addition, we have both expanded and extended existing studies
of surufatinib and fruquintinib in the U.S. ahead of upcoming
regulatory authority end of Phase II meetings. This will move
certain start-up costs of our global Phase II/III registration
studies on surufatinib and fruquintinib into 2020.
2019 Previous Guidance 2019 Current
Guidance Adjustments
------------------------------------------------------- ---------------------- ---------------------- -------------
Adjusted R&D Expenses $(160) - (200) million $(130) - (170) million $(30) million
Adjusted Group Net Cash Flows excluding financing $(120) - (150) million $(90) - (120) million $(30) million
activities
------------------------------------------------------- ---------------------- ---------------------- -------------
Use of Non-GAAP Financial Measures - References in this
announcement to adjusted R&D expenses, adjusted Group net cash
flows and adjusted Group net cash flows excluding financing
activities and financial measures reported at CER are based on
non-GAAP financial measures. Please see the "Use of Non-GAAP
Financial Measures and Reconciliation" below for further
information relevant to the interpretation of these financial
measures and reconciliations of these financial measures to the
most comparable GAAP measures.
About Chi-Med
Chi-Med (AIM/Nasdaq: HCM) is an innovative biopharmaceutical
company which researches, develops, manufactures and markets
pharmaceutical products. Its Innovation Platform, Hutchison
MediPharma, has about 440 scientists and staff focusing on
discovering, developing and commercializing targeted therapeutics
and immunotherapies in oncology and autoimmune diseases. It has a
portfolio of eight cancer drug candidates currently in clinical
studies around the world. Chi-Med's Commercial Platform
manufactures, markets, and distributes prescription drugs and
consumer health products, covering an extensive network of
hospitals across China.
Chi-Med is headquartered in Hong Kong and is dual-listed on the
AIM market of the London Stock Exchange and the Nasdaq Global
Select Market. For more information, please visit:
www.chi-med.com.
CONTACTS
Investor Enquiries
Mark Lee, Senior Vice President +852 2121 8200
Annie Cheng, Vice President +1 (973) 567 3786
David Dible, Citigate Dewe Rogerson +44 7967 566 919 (Mobile)
david.dible@citigatedewerogerson.com
Xuan Yang, Solebury Trout +1 (415) 971 9412 (Mobile)
xyang@troutgroup.com
Media Enquiries
UK & Europe - Anthony Carlisle, Citigate Dewe Rogerson +44 7973 611 888 (Mobile)
anthony.carlisle@cdrconsultancy.co.uk
Americas - Brad Miles, Solebury Trout +1 (917) 570 7340 (Mobile)
bmiles@troutgroup.com
Hong Kong & Asia ex-China - Joseph Chi Lo, Brunswick +852 9850 5033 (Mobile)
jlo@brunswickgroup.com
- Zhou Yi, Brunswick +852 9783 6894 (Mobile)
yzhou@brunswickgroup.com
Mainland China - Sam Shen, Edelman +86 136 7179 1029 (Mobile)
sam.shen@edelman.com
Nominated Advisor
Richard Gray / Atholl Tweedie, Panmure Gordon (UK) Limited +44 (20) 7886 2500
References
Unless the context requires otherwise, references in this
announcement to the "Group," the "Company," "Chi-Med," "Chi-Med
Group," "we," "us," and "our," mean Hutchison China MediTech
Limited and its consolidated subsidiaries and joint ventures unless
otherwise stated or indicated by context.
Past Performance and Forward-Looking Statements
The performance and results of operations of the Group contained
within this announcement are historical in nature, and past
performance is no guarantee of future results of the Group. This
announcement contains forward-looking statements within the meaning
of the "safe harbor" provisions of the U.S. Private Securities
Litigation Reform Act of 1995. These forward-looking statements can
be identified by words like "will," "expects, " "anticipates,"
"future," "intends," "plans," "believes," "estimates," "pipeline,"
"could," "potential," "believe," "first-in-class," "best-in-class,"
"designed to," "objective," "guidance," "pursue," or similar terms,
or by express or implied discussions regarding potential drug
candidates, potential indications for drug candidates, a potential
SEHK listing and concurrent global offering of our securities or by
discussions of strategy, plans, expectations or intentions. You
should not place undue reliance on these statements. Such
forward-looking statements are based on the current beliefs and
expectations of management regarding future events, and are subject
to significant known and unknown risks and uncertainties. Should
one or more of these risks or uncertainties materialize, or should
underlying assumptions prove incorrect, actual results may vary
materially from those set forth in the forward-looking statements.
There can be no guarantee that any of our drug candidates will be
approved for sale in any market, or that any approvals which are
obtained will be obtained at any particular time, or that any such
drug candidates will achieve any particular revenue or net income
levels. In particular, management's expectations could be affected
by, among other things: unexpected regulatory actions or delays or
government regulation generally; the uncertainties inherent in
research and development, including the inability to meet our key
study assumptions regarding enrollment rates, timing and
availability of subjects meeting a study's inclusion and exclusion
criteria and funding requirements, changes to clinical protocols,
unexpected adverse events or safety, quality or manufacturing
issues; the inability of a drug candidate to meet the primary or
secondary endpoint of a study; the inability of a drug candidate to
obtain regulatory approval in different jurisdictions or gain
commercial acceptance after obtaining regulatory approval; global
trends toward health care cost containment, including ongoing
pricing pressures; uncertainties regarding actual or potential
legal proceedings, including, among others, actual or potential
product liability litigation, litigation and investigations
regarding sales and marketing practices, intellectual property
disputes, and government investigations generally; and general
economic and industry conditions, including uncertainties regarding
the effects of the persistently weak economic and financial
environment in many countries and uncertainties regarding future
global exchange rates. For further discussion of these and other
risks, see Chi-Med's filings with the U.S. Securities and Exchange
Commission and on AIM. Chi-Med is providing the information in this
announcement as of this date and does not undertake any obligation
to update any forward-looking statements as a result of new
information, future events or otherwise.
In addition, this announcement contains statistical data and
estimates that Chi-Med obtained from industry publications and
reports generated by third-party market research firms. Although
Chi-Med believes that the publications, reports and surveys are
reliable, Chi-Med has not independently verified the data and
cannot guarantee the accuracy or completeness of such data. You are
cautioned not to give undue weight to this data. Such data involves
risks and uncertainties and are subject to change based on various
factors, including those discussed above.
Inside Information
This announcement contains inside information for the purposes
of Article 7 of Regulation (EU) No 596/2014.
Ends
Financial Review
Chi-Med Group revenue for the six months ended June 30, 2019 was
$102.2 million (H1-18: $102.2m). Revenue from the Commercial
Platform increased to $90.2 million (H1-18: $88.6m) driven mainly
by continued progress on our Hutchison Sinopharm business. Revenue
from the Innovation Platform decreased to $12.0 million in the
first half of 2019 (H1-18: $13.6m), reflecting a transitioning from
a focus on earning service fees from our partners through
development collaborations to reporting product sales revenue and
royalty income from the commercial launch of our innovations such
as Elunate(R) .
It should be noted that Group revenues do not include the
revenues of our two large-scale, 50/50 joint ventures in China,
Shanghai Hutchison Pharmaceuticals Limited ("SHPL") and Hutchison
Whampoa Guangzhou Baiyunshan Chinese Medicine Company Limited
("HBYS"), since these are accounted for using the equity
method.
In the first half of 2019, our Commercial Platform, which is a
material source of profit and cash for Chi-Med, recorded an
operating profit of $30.8 million (H1-18: $31.0m). This reflected
growth in SHPL's coronary artery disease business offset by the
halt of service fees from Seroquel(R) and weakening of the RMB
against the U.S. dollar. The Innovation Platform incurred an
operating loss of $63.9 million (H1-18: operating loss of $53.1m)
as a result of progress on virtually all aspects of our R&D
operations in support of our pipeline of eight novel drug
candidates.
Net corporate unallocated expenses, primarily Chi-Med Group
overhead and operating costs, increased to $7.3 million (H1-18:
$4.9m) mainly due to organizational expansion and increased
professional fees associated with preparations for our potential
listing on The Stock Exchange of Hong Kong Limited ("SEHK").
Consequently, Chi-Med Group's operating loss was $40.3 million
(H1-18: operating loss of $27.0m).
The aggregate of interest and income tax expenses of Chi-Med
Group, as well as net income attributable to non-controlling
interests was $5.0 million (H1-18: $5.7m).
The resulting total Group net loss attributable to Chi-Med was
$45.4 million (H1-18: net loss of $32.7m).
As a result, Group net loss attributable to Chi-Med in the first
half of 2019 was $0.07 per ordinary share / $0.34 per American
depositary share ("ADS"), compared to net loss attributable to
Chi-Med of $0.05 per ordinary share / $0.25 per ADS, in H1
2018.
Cash and Financing
We have used, and will continue to use, financial discipline in
aiming to partially offset increasing clinical investment with cash
generated in our operating activities. This includes cash from
dividends paid by our non-consolidated Commercial Platform joint
ventures, collaboration payments received from our multinational
pharmaceutical company partners, and now increasingly net income,
manufacturing and royalty revenues from our launched products.
These cash inflows offset a material portion of our R&D
expenses, and as a result, total Chi-Med Group net cash flows,
excluding financing activities, during the first half of 2019 was
-$34.2 million despite R&D expenses of $74.5 million, both on
an as adjusted (non-GAAP) basis.
As of June 30, 2019, we had available cash resources of $383.6
million (December 31, 2018: $420.3m) at the Chi-Med Group level.
This included cash and cash equivalents and short-term investments
of $237.3 million (December 31, 2018: $301.0m) and unutilized bank
borrowing facilities of $146.3 million (December 31, 2018:
$119.3m). In addition, as of June 30, 2019, our non-consolidated
joint ventures (SHPL, HBYS and Nutrition Science Partners Limited)
held $64.0 million (December 31, 2018: $59.2m) in available cash
resources.
Outstanding bank loans, at the Chi-Med Group level, as of June
30, 2019 amounted to nil (December 31, 2018: $26.7m). Also, as of
June 30, 2019, our non-consolidated joint ventures had no
outstanding bank loans.
Equity Capital Markets ("ECM") update
In mid-April 2019, Chi-Med announced our proposed intention to
list our shares on the SEHK. We continue to consider this however,
our listing application and potential concurrent global offering
remain subject to, among other things, market conditions.
In July 2019, our largest shareholder CK Hutchison(1) completed
most of its previously announced plan to reduce its shareholding in
Chi-Med to below 50% by reducing its shareholding from 60.2% to
51.2%. Upon the shareholding of CK Hutchison in Chi-Med falling
below 50%, Chi-Med will no longer be a consolidated subsidiary of
CK Hutchison thereby reducing the impact on CK Hutchison's earnings
of Chi-Med's investment in the accelerated development of its
global pipeline. Going forward CK Hutchison is expected to remain
Chi-Med's largest shareholder for the foreseeable future and
Chi-Med will continue to benefit from the long term support of its
founding shareholder.
We believe that our current cash resources including short-term
investments, along with our cash flow from operations, dividend
payments and potential bank borrowings, are sufficient for Chi-Med
to reach multiple value inflection points on our pipeline. We also
have the added potential to access non-dilutive finance that could
be derived from the disposal of certain non-core Commercial
Platform assets.
This provides us with considerable flexibility on the type, and
timing, of any future ECM activities.
([1]) CK Hutchison Holdings Limited ("CK Hutchison") (SEHK: 1),
a multinational conglomerate with revenues of $58 billion in 2018
and employing over 300,000 people in over 50 countries across the
world.
Operations Review
Innovation Platform
Chi-Med's pipeline of novel drug candidates has been created and
developed by our Innovation Platform, an in-house R&D operation
which was started in 2002. Since then, we have built a large team
of about 440 scientists and staff (December 31, 2018: 420) based
mainly in China. We operate a fully-integrated drug discovery and
development operation covering chemistry, biology, pharmacology,
toxicology, chemistry and manufacturing controls for clinical and
commercial supply, clinical and regulatory and other functions.
Looking ahead, we plan to further expand and leverage this platform
to produce and commercialize a stream of novel drug candidates with
global potential that can improve the treatment of patients with
cancer and autoimmune diseases globally.
Innovation Platform revenue in H1 2019 was $12.0 million (H1-18:
$13.6m) mainly from service fee payments from AstraZeneca and Lilly
in addition to initial product revenue and royalties from
Elunate(R) . We are gradually transitioning the revenue model of
our Innovation Platform from a fee for service model, in which
Chi-Med provided multi-national partners services associated with
research and clinical development, to one focused on generating
revenues from product sales and royalty income from our innovative
drugs.
Net loss attributable to Chi-Med increased to $63.8 million
(H1-18: net loss of $52.9m) as a result of increased R&D
expenses of $74.5 million (H1-18: $66.7m) on an as adjusted
(non-GAAP) basis driven by progress on virtually all aspects of our
R&D operations in support of our pipeline of eight drug
candidates.
Since inception, the Innovation Platform has dosed over 4,800
patients/subjects, with over 400 in H1 2019, in clinical trials of
our drug candidates in over 30 active or completed studies.
Product Pipeline Progress
Savolitinib (AZD6094)
Savolitinib is a potent and selective inhibitor of MET, an
enzyme which has been shown to function abnormally in many types of
solid tumors. In clinical studies to date in over 1,000 patients
globally, savolitinib has shown promising signs of clinical
efficacy in patients with MET gene alterations in lung cancer,
kidney cancer, and gastric cancer with an acceptable safety
profile.
We are currently testing savolitinib in global partnership with
AstraZeneca, both as a monotherapy and in combinations. Two ongoing
studies, which subject to positive clinical outcome, are designed
to support NDA submission in lung cancer. Several additional
studies, mostly proof-of-concept, have reported or will report in
2019 and subject to outcomes could warrant further development.
Savolitinib - Lung cancer: MET is an increasingly important
target in NSCLC. The table below shows a summary of the clinical
studies for savolitinib in lung cancer patients.
Treatment Name, Line, Patient Sites Phase Status/Plan NCT #
Focus
======================= ===================== ====== =============== ===================== ===========
Savolitinib monotherapy MET Exon 14 deletion China II Registration Target enrollment NCT02897479
completed
======================= ===================== ====== =============== ===================== ===========
Savolitinib and TATTON: 2L/3L EGFRm+; Global Ib/II Completed enrollment; NCT02143466
Tagrisso(R) EGFR TKI refractory; preliminary
MET+ data presented
at AACR 2019
======================= ===================== ====== =============== ===================== ===========
Savolitinib and SAVANNAH: 2L/3L Global II (potential Initiated in NCT03778229
Tagrisso(R) EGFRm+; Tagrisso(R) registration) Dec 2018
refractory; MET+
======================= ===================== ====== =============== ===================== ===========
Savolitinib and 2L EGFRm; Iressa(R) China Ib/II Completed NCT02374645
Iressa(R) ref; MET+
======================= ===================== ====== =============== ===================== ===========
MET Exon 14 deletion NSCLC (NCT02897479) - It is estimated that
2-3% of NSCLC patients have MET Exon 14 deletion, which is believed
to play an important role in driving tumor growth.
Recent data from the 2019 ASCO Meeting showed that two selective
MET inhibitors in development outside of China, capmatinib and
tepotinib, had an overall ORR ranging from 41% to 68% in clinical
studies in MET Exon 14 deletion NSCLC patients. Xalkori(R) , a
multi-kinase inhibitor with MET inhibitory activity, demonstrated a
lower ORR of approximately 32% in clinical studies.
We are conducting a Phase II registration intent study of
savolitinib as a monotherapy for MET Exon 14 deletion NSCLC
patients who have progressed following prior systemic therapy, or
unable to receive chemotherapy. During 2019 AACR, interim data were
presented on 41 treated patients, of which only 31 patients were
efficacy evaluable. The overall data was encouraging, with efficacy
in-line with other selective MET inhibitors, supporting the
continuation of the study as originally planned. Treatment emergent
CTC grade >=3 adverse events with greater than 5% incidence
related to savolitinib treatment were increased aspartate
aminotransferase (7%) and increased alanine aminotransferase (7%).
We have now reached our enrollment goal for this Phase II
registration study, and subject to clinical outcome later this
year, this indication has high potential to be savolitinib's first
NDA in H1 2020.
Tagrisso(R) (osimertinib) resistance in NSCLC: Since its U.S.
Food and Drug Administration (FDA) approval in November 2015,
Tagrisso(R) has been established as an important treatment for EGFR
mutation positive NSCLC and has now been approved in over 80
countries. Tagrisso(R) global sales were $1.9 billion in 2018, its
third year since launch, and $1.4 billion in the first half of 2019
making it AstraZeneca's highest selling medicine.
Given the significant use of Tagrisso(R) for EGFR mutation
positive NSCLC, understanding the mechanism of acquired resistance,
following Tagrisso(R) treatment, is a key clinical question to
inform the next treatment choice.
At the European Society of Medical Oncology Congress in 2018,
AstraZeneca presented data on the acquired resistance spectrum
detected in circulating tumor cells in patient plasma after
progression on Tagrisso(R) when used in the first-line (FLAURA) and
second-line T790M (AURA3) Phase III studies. MET amplification was
the most frequent mechanism of acquired resistance to Tagrisso(R) ,
with 15% of patients in the FLAURA study, and 19% of patients in
AURA3 study exhibiting MET amplification after treatment with
Tagrisso(R) .
TATTON study (Part B) and TATTON study (Part D); Phase Ib/II
expansion studies of savolitinib in combination with Tagrisso(R) in
NSCLC EGFR mutation positive TKI refractory patients (NCT02143466)
- In 2016, we initiated a global Phase Ib/II expansion study in
NSCLC, the TATTON (Part B) study, aiming to recruit sufficient MET
gene amplified patients who had progressed after prior treatment
with EGFR inhibitors to support a decision on global Phase II/III
registration strategy.
First-generation EGFR TKI, such as Iressa(R) and Tarceva(R) ,
refractory patients with acquired resistance driven by MET
amplification
In March 2019, preliminary TATTON (Part B) data were presented
at AACR 2019 aimed at expanding and corroborating preliminary data
presented at the World Conference on Lung Cancer ("WCLC") in 2017.
The AACR 2019 presentation also included median duration of
response data for the first time, since it was not mature at the
time of WCLC 2017. Data for the savolitinib in combination with
Tagrisso(R) was presented for a total of 43 evaluable patients (46
total patients) who were T790M- and who had not previously received
a third-generation EGFR inhibitor. There were 24 confirmed
responses (56% of efficacy evaluable patients), four unconfirmed
responses, 12 other patients with stable disease, for a total of 40
patients who experienced disease control (93% of efficacy evaluable
patients). The median duration of response was 7.1 months, with an
interquartile range from 4.1 months to 10.7 months. CTC grade
>=3 adverse events with greater than 5% incidence independent of
causality were increased aspartate aminotransferase (8%), increased
neutrophil count (8%), fatigue (7%) and pain (7%).
In late 2017, the TATTON study (Part D) was initiated to study
Tagrisso(R) combined with a lower savolitinib dose (300 mg once
daily) in the context of maximizing long-term tolerability of the
combination. Enrollment has now been completed, patients continue
to be treated and clinical data continues to mature.
Tagrisso(R) or another experimental third-generation EGFR TKI
refractory patients with acquired resistance driven by MET
amplification
Also in March 2019 at AACR, further TATTON (Part B) preliminary
data, for the savolitinib in combination with Tagrisso(R) , were
presented for a total of 39 evaluable patients, that had progressed
on Tagrisso(R) monotherapy and harbored MET amplification. There
were 12 confirmed responses (31% of evaluable patients), five
unconfirmed responses and 16 patients with stable disease, totaling
33 patients who experienced disease control (85% of efficacy
evaluable patients). The median duration of response was 9.7
months, with an interquartile range from 5.5 months to an
incalculable higher figure at the time of data cut-off. Overall the
combination regimen of savolitinib and Tagrisso(R) was tolerable
with the only CTC grade >=3 adverse event with greater than 5%
incidence independent of causality was decreased appetite (6%).
SAVANNAH (NCT03778229) - Based on the encouraging results of the
multiple TATTON studies, AstraZeneca has initiated a global Phase
II study of savolitinib / Tagrisso(R) combination in EGFR mutation
positive NSCLC patients who have progressed following first or
second-line Tagrisso(R) therapy due to MET amplification - The
SAVANNAH study is a single-arm study, in North and South America,
Europe and Asia, targeting an interim analysis and regulatory
agency discussion in mid-2020 which will guide registration
strategy for this indication.
Savolitinib / Iressa(R) combination (NCT02374645) - Separately,
a Phase Ib study combining AstraZeneca's first-generation EGFR TKI
Iressa(R) with savolitinib has been completed in China. Chi-Med and
AstraZeneca are evaluating this opportunity in the context of the
evolving treatment paradigm for EGFRm NSCLC.
Savolitinib - Kidney cancer: The table below shows a summary of
the clinical studies for savolitinib in kidney cancer patients.
Treatment Name, Line, Patient Sites Phase Status/Plan NCT #
Focus
=============== ========================== ======== ===== ============ ===========
Savolitinib and CALYPSO: Papillary UK/Spain II Interim - NCT02819596
Imfinzi(R) RCC Presented
at ASCO GU
2019
=============== ========================== ======== ===== ============ ===========
Savolitinib and CALYPSO: Clear cell UK/Spain II Enrolling NCT02819596
Imfinzi(R) RCC; VEGFR TKI refractory - Data late
2019/early
2020
=============== ========================== ======== ===== ============ ===========
Savolitinib and Immunotherapy Combinations - Immunotherapy
combinations are rapidly changing the treatment landscape in kidney
cancer. Anti-PD-L1 antibodies have been associated with clinical
benefits in metastatic RCC, and MET dysregulation has been
considered to play an important role in the pathogenesis of RCC.
Moreover, it is believed that the MET signaling pathway may have a
complex interplay with the immune system through recruitment of
immune suppressive cells such as neutrophils.
CALYPSO Phase II in RCC of savolitinib with Imfinzi(R) PD-L1
inhibitor combination (NCT02819596) - The CALYPSO study is an
investigator initiated open-label Phase I/II study of savolitinib
in combination with Imfinzi(R) , an anti-PD-L1 antibody owned by
AstraZeneca. The study is evaluating treatment of PRCC and clear
cell RCC patients at sites in the U.K. and Spain.
PRCC cohort - Interim data for the PRCC cohort of the CALYPSO
Phase II study were presented at 2019 ASCO GU showing encouraging
efficacy across all PRCC patients (with or without MET
amplification). The interim CALYPSO data, reported ORR of 27%
(11/41), while median PFS was 5.3 months (95% CI: 1.5-12.0 months).
Median OS was immature/not reached. For previously untreated
patients (n=28), ORR was 32% (9/28). The combination was tolerable
with edema (10%), nausea (5%), and transaminitis (5%) being most
frequent treatment related Grade >=3 adverse events. The
investigators concluded that the Imfinzi(R) / savolitinib
combination is associated with encouraging clinical efficacy and
durable responses in PRCC. The CALYPSO study continues, with
further data expected to be presented at an upcoming scientific
conference in 2020.
Savolitinib - Gastric cancer: Multiple Phase II studies have
been conducted in Asia to study savolitinib in MET-driven gastric
cancer patients. A total of well over 1,000 gastric cancer patients
had been screened in these studies and those patients with
confirmed MET-driven disease were treated. The table below shows a
summary of our clinical trials for savolitinib in gastric cancer
patients.
Treatment Name, Line, Patient Sites Phase Status/Plan NCT #
Focus
================ ============================= ============ ===== =================== ==============
Savolitinib Gastric cancer China & Ib/II Completed in NCT01985555
monotherapy (MET amplification) South Korea China; VIKTORY / NCT02449551
and VIKTORY (in complete;
South Korea) to publish
2019
================ ============================= ============ ===== =================== ==============
Savolitinib VIKTORY: Gastric South Korea II Enrollment stopped NCT02447406
and Taxotere(R) cancer (MET amplification) (Patients directed
to savolitinib
mono due to
high efficacy
observed)
================ ============================= ============ ===== =================== ==============
Savolitinib VIKTORY: Gastric South Korea II NCT02447380
and Taxotere(R) cancer (MET over-expression)
================ ============================= ============ ===== =================== ==============
Savolitinib monotherapy in MET amplified gastric cancer patients
(NCT01985555 / NCT02449551) - Preliminary results were presented at
the Chinese Society of Clinical Oncology conference in late 2017
for the efficacy evaluable MET gene amplified patients in China.
This China study concluded that savolitinib monotherapy
demonstrated promising anti-tumor efficacy in gastric cancer
patients with MET gene amplification, and the potential benefit to
these patients clearly warranted further exploration.
The South Korean study, known as VIKTORY, and is an umbrella
study with MET amplification as one of its cohorts, is run and
sponsored by the Samsung Medical Center in South Korea. The VIKTORY
Phase II study is now complete and the full data set is expected to
be published in a scientific journal in 2019.
Savolitinib - Prostate cancer: The table below shows a summary
of the clinical study for savolitinib in prostate cancer
patients.
Treatment Name, Line, Patient Sites Phase Status/Plan NCT #
Focus
======================= =============================== ====== ===== =========== ===========
Savolitinib monotherapy Metastatic Castration-Resistant Canada II Enrolling NCT03385655
Prostate Cancer
======================= =============================== ====== ===== =========== ===========
This study is an umbrella study and is sponsored by the Canadian
Cancer Trials Group. The study targets to enroll approximately 500
patients with savolitinib being one of four cohorts.
Fruquintinib (Elunate(R) )
Fruquintinib is a highly selective and potent oral inhibitor of
VEGFR 1/2/3 that was designed to be a global best-in-class VEGFR
inhibitor for many types of solid tumors. VEGFR inhibitors play a
pivotal role in tumor-related angiogenesis, cutting off the blood
supply that a tumor needs to grow rapidly.
Fruquintinib was designed to improve kinase selectivity in
comparison to other approved small molecule TKIs, to minimize
off-target toxicities, improve tolerability and provide more
consistent target coverage. The high tolerability in patients to
date, along with fruquintinib's low potential for drug-drug
interaction based on preclinical assessment, suggests that it may
be highly suitable for combinations with other anti-cancer
therapies.
The global market for anti-angiogenesis therapies was estimated
at over $16 billion in 2018, including both monoclonal antibodies
and small molecules approved in around 30 tumor settings.
Chi-Med retains all rights to fruquintinib outside of China and
is partnered with Lilly in China.
The table below shows a summary of the clinical studies for
fruquintinib.
Treatment Name, Line, Patient Sites Phase Status/Plan NCT #
Focus
======================== ============================== ===== ===== ==================== ===========
Fruquintinib monotherapy FRESCO: >=3L CRC; chemotherapy China III Approved and NCT02314819
refractory launched
======================== ============================== ===== ===== ==================== ===========
Fruquintinib monotherapy 3L/4L CRC; Stivarga(R) US/EU Ib US/EU Ph.II/III NCT03251378
/Lonsurf(R) ref./intol. registration
study in planning
======================== ============================== ===== ===== ==================== ===========
Fruquintinib and FRUTIGA: 2L gastric China III Enrolling; Interim NCT03223376
paclitaxel cancer analysis conducted
in early 2019
======================== ============================== ===== ===== ==================== ===========
Fruquintinib monotherapy FALUCA: 3L NSCLC; chemotherapy China III Completed. Failed NCT02691299
refractory to meet primary
endpoint
======================== ============================== ===== ===== ==================== ===========
Fruquintinib and 1L NSCLC; EGFRm China II Enrollment completed NCT02976116
Iressa(R)
======================== ============================== ===== ===== ==================== ===========
Fruquintinib and 2L metastatic CRC/NSCLC China Ib Enrolling NCT03977090
genolimzumab (PD-1)
======================== ============================== ===== ===== ==================== ===========
Fruquintinib and Solid tumors China Ib/II Enrolling NCT03903705
Tyvyt(R) (PD-1)
======================== ============================== ===== ===== ==================== ===========
Fruquintinib and Solid tumors US I In planning TBD
Tyvyt(R) (PD-1)
======================== ============================== ===== ===== ==================== ===========
Fruquintinib - Colorectal Cancer:
Fruquintinib capsules, sold under the brand name Elunate(R) ,
were approved for marketing in China by the National Medical
Products Administration ("NMPA") in September 2018 and commercially
launched by Lilly in late November 2018. Elunate(R) is for the
treatment of patients with metastatic CRC that have been previously
treated with fluoropyrimidine, oxaliplatin and irinotecan,
including those who have previously received anti-VEGF therapy
and/or anti-EGFR therapy (RAS wild type).
Elunate(R) launch update:
Pricing - Elunate(R) was launched with an initial retail price
of RMB21,960 ($3,260) per cycle, on a four-week per cycle basis
paid for out-of-pocket by patients in China. To broaden access to
Elunate(R) , Lilly has implemented a means-based patient access
program, whereby patients pay for three 28-day cycles of Elunate(R)
(cycles one, two and five) at the full price. Outside of these
three paid-for cycles, Elunate(R) is provided for at no cost.
Reimbursement - During the first half of 2019 both Lilly and
Chi-Med have been actively working to expand government
reimbursement of Elunate(R) in China. In early 2019 Elunate was
included in the reimbursement list for Zhuhai, a city of 1.6
million people, and in June 2019 it was included into the Shanghai
provincial reimbursement drug list covering 15.0 million
patients.
More importantly, we are now focused on potentially trying to
secure inclusion in the next update of the NRDL which is expected
to be finalized in early Q4 2019. Inclusion in the NRDL would
trigger distribution of Elunate(R) in all state-run hospital
pharmacies in China and open up reimbursement for the over 317
million people included in the main medical insurance program for
urban employees in China.
In-market Sales performance - Sales of Elunate(R) , as provided
by Lilly, totaled $11.4 million (RMB77.1 million) in the first half
of 2019 (H1-2018: nil) resulted primarily from out-of-pocket
payments from patients with support via the means-tested patient
access program.
This represents first six-month revenue for Elunate(R) that is
well ahead, at the same stage, of the five small molecule VEGFR
inhibitors previously launched by multinational companies in China.
These products, all reported on a CER basis, include: Nexavar(R)
(sorafenib, Bayer AG) launched in 2006 with 2007 sales of $18.6
million (RMB125.1m); Sutent(R) (sunitinib, Pfizer, Inc.), launched
in 2007 with 2008 sales of $7.4 million (RMB49.9m); Inlyta(R)
(axitinib, Pfizer, Inc.), launched in 2015 with 2016 sales of $12.1
million (RMB81.6m); Votrient(R) (pazopanib, Novartis International
AG), launched in 2017 with 2018 sales of $12.5 million (RMB84.0m);
and Stivarga(R) (regorafenib, Bayer AG), launched in 2017 with
first six-month sales of $4.7 million (RMB32.0m) and 2018 sales of
$21.2 million (RMB142.7m).
Chi-Med Revenues in H1 2019 from Elunate(R) - Chi-Med receives
four types of revenue from Lilly associated with Elunate(R) : (1)
manufacturing product sales; (2) royalties; (3) fees for
development-related services; and (4) reimbursement of development
costs of certain initial indications. With the commercial launch of
Elunate(R) we are transitioning to a model in which our main
revenues from Lilly will be manufacturing product sales and
royalties. During the first half of 2019, Chi-Med reported revenues
from Lilly totaling $6.1 million (H1-18: $6.0m) including
manufacturing product sales of $3.0 million (H1-18: nil); royalties
of $1.7 million (H1-18: nil); service fees of $0.8 million (H1-18:
$1.1m); and clinical trial cost reimbursement of $0.6 million
(H1-18: $4.9m).
Outlook for Elunate(R) in colorectal cancer (CRC) - Elunate(R)
's main competitor in third-line CRC in China is Stivarga(R)
(regorafenib), a first generation small molecule multi-kinase
inhibitor, from Bayer AG. Stivarga(R) in-market sales in China,
which were $21.2 million in the whole of 2018, increased rapidly to
$19.7 million (RMB133m) in Q1 2019. Growth was likely as a result
of its inclusion in the NRDL in October 2018, and entry into
hospital pharmacies, as well as its approval in second-line
hepatocellular carcinoma in March 2018.
The efficacy and safety-profile advantages for Elunate(R) over
Stivarga(R) in third-line CRC are well documented, with Stivarga(R)
carrying a black-box safety warning for liver toxicity in the
United States. In the FRESCO study, Elunate(R) demonstrated a
tolerable liver safety profile which could be very important for
advanced CRC patients, particularly the high proportion of those
with liver metastases. Furthermore, patients in the FRESCO study
who had prior exposure to anti-VEGF therapies derived robust
benefit from Elunate(R) treatment, a clear point of differentiation
as compared to Stivarga(R) .
Global development of fruquintinib in CRC - We are currently
enrolling a Phase Ib study in the U.S. and have begun planning for
a Phase II/III registration study in the United States and Europe
in third or fourth-line metastatic CRC patients who are resistant
to or intolerant of prior treatment with Stivarga(R) or Lonsurf(R)
(a cytotoxic chemotherapy agent approved in third-line CRC in
various countries excluding China). We expect to begin this study
in 2020.
Fruquintinib - Gastric Cancer:
Phase III study of fruquintinib in combination with paclitaxel
in gastric cancer (second-line) (NCT03223376) - In October 2017, we
initiated the FRUTIGA study, a randomized, double-blind, Phase III
study in China to evaluate the efficacy and safety of fruquintinib
combined with paclitaxel compared with paclitaxel monotherapy for
second-line treatment of advanced gastric cancer. Over 500 patients
are expected to be enrolled into the FRUTIGA study at a 1:1 ratio
with the primary endpoint of this study being OS. Enrollment is
expected to be completed in mid-2020 with top line results in early
2021.
In April 2019, we conducted an interim analysis of the FRUTIGA
study for futility. The analysis evaluated PFS and OS trends after
six months of therapy for the first 100 patients recruited into the
study. The IDMC recommended to continue the study without
changes.
Fruquintinib - NSCLC:
Phase III study of fruquintinib monotherapy in third-line NSCLC
(NCT02691299) - In November 2018, we announced the outcome of
FALUCA, the Phase III trial of fruquintinib in advanced NSCLC
patients in China who have failed two lines of systemic
chemotherapy. The trial did not meet the primary endpoint to
demonstrate a statistically significant increase in OS compared to
placebo. However, fruquintinib demonstrated a statistically
significant improvement in all secondary endpoints including PFS,
ORR, disease control rate ("DCR") and duration of response as
compared to the placebo. The safety profile of the trial was in
line with that observed in prior clinical studies. We intend to
present a detailed analysis of the study in September at WCLC 2019
in Barcelona, Spain.
Phase II study of fruquintinib in combination with Iressa(R) in
first-line NSCLC (NCT02976116) - In early 2017, we initiated a
multi-center, single-arm, open-label, dose-finding Phase II study
of fruquintinib in combination with Iressa(R) in China in the
first-line setting for patients with advanced or metastatic NSCLC
with EGFR activating mutations. We have enrolled about 50 patients
in this study with the objective of evaluating the safety and
tolerability as well as the efficacy of the combination
therapy.
Preliminary interim data for this study were presented in late
2017 at WCLC, showing an encouraging response and safety profile.
Fruquintinib's safety and tolerability profile, resulting from its
high kinase selectivity, combined with better flexibility to manage
treatment emergent toxicities due to its shorter half-life than
monoclonal antibody anti-angiogenesis therapies, makes it a
suitable combination partner for EGFR TKIs. The primary objective
of this exploratory study is to determine the safety and
tolerability and median PFS of the fruquintinib and Iressa(R)
combination. The study is now complete and we expect to submit data
for presentation at an upcoming scientific conference.
Fruquintinib - Combinations with Checkpoint Inhibitors:
In November 2018, we entered into two collaboration agreements
to evaluate the safety, tolerability and efficacy of fruquintinib
in combination with checkpoint inhibitors. These include a global
collaboration with Innovent to evaluate the combination of
fruquintinib with Innovent's Tyvyt(R) (sintilimab, IBI308), a PD-1
monoclonal antibody approved in China in late 2018 and a China
collaboration with Genor to evaluate the fruquintinib combination
with genolimzumab (GB226), a PD-1 monoclonal antibody being
developed by Genor. Phase I studies have now been initiated to
establish the safe and effective dose regimens for the fruquintinib
combinations with either Tyvyt(R) or genolimzumab,
respectively.
SuRUfatinib (HMPL-012 or sulfatinib)
Surufatinib is an oral small molecule angio-immuno kinase
inhibitor targeting VEGFR 1, 2 and 3, FGFR1 and CSF-1R kinases that
may simultaneously block tumor angiogenesis and immune evasion. Its
angio-immuno kinase profile seems to support surufatinib as an
attractive candidate for exploration of possible combinations with
checkpoint inhibitors against various cancers.
Chi-Med currently retains all rights to surufatinib
worldwide.
Surufatinib, as a monotherapy, is in proof-of-concept clinical
trials in the U.S. and late-stage clinical trials in China. A
summary of these clinical studies is shown in the table below.
Treatment Name, Line, Patient Sites Phase Status/Plan NCT #
Focus
======================= ======================== ===== ====== ===================== ===========
Surufatinib monotherapy SANET-ep: Non-pancreatic China III Met primary endpoint; NCT02588170
NET preparing NDA
======================= ======================== ===== ====== ===================== ===========
Surufatinib monotherapy SANET-p: Pancreatic China III Interim analysis NCT02589821
NET early 2020
======================= ======================== ===== ====== ===================== ===========
Surufatinib monotherapy 2L Pancreatic NET; US/EU Ib US/EU Ph.II/III NCT02549937
Sutent(R) /Afinitor(R) registration study
refractory in planning
======================= ======================== ===== ====== ===================== ===========
Surufatinib monotherapy Chemotherapy refractory China II/III Enrolling NCT03873532
BTC
======================= ======================== ===== ====== ===================== ===========
Surufatinib and Solid tumors US I In planning TBD
Tuoyi(R) (PD-1)
======================= ======================== ===== ====== ===================== ===========
Surufatinib and Solid tumors China I Enrolling NCT03879057
Tuoyi(R) (PD-1)
======================= ======================== ===== ====== ===================== ===========
Surufatinib - Neuroendocrine Tumors (NET):
NETs begin in the specialized cells of the body's neuroendocrine
system. Cells have traits of both hormone-producing endocrine cells
and nerve cells. NETs are found throughout the body's organ system
and have a highly complex and fragmented epidemiology with
approximately 55-75% of NETs originating in the gastro-entero
pancreatic ("GEP") system of the gastrointestinal tract and
pancreas, 25-30% originate in the lung or bronchus, and a further
10-20% originate from other or unknown origins.
There were 19,000 newly diagnosed cases of NET in the U.S. in
2018. Importantly, NETs are associated with a relatively long
duration of survival compared to other tumors. As a result, there
were approximately 141,000 estimated patients living with NETs in
the U.S. in 2018. Of this number, up to 90%, or approximately
132,000, were non-pancreatic NET patients.
In China there were approximately 67,600 newly diagnosed NET
patients in 2018 and, while no prevalence data exists in China,
considering the U.S. incidence to prevalence ratio, there could be
as many as 490,000 patients living with the disease. Until such
time as NET patients in China are diagnosed earlier and given
broader access to treatment options we expect that estimated
Prevalence to Incidence ratio in China will likely be lower than
that currently observed in the U.S.
NETs can be functional, releasing hormones and peptides that
cause symptoms like diarrhea and flushing, or non-functional with
no symptoms, but on a high level, NET is classified as either
early- or advanced-disease.
Early NETs are generally functional and well-differentiated,
looking like healthy cells, growing slowly with a low Mitotic count
(mitosis is process by which tumor cells grow and divide) and a low
Ki-67 index (Ki-67 is a protein that increases as cells divide).
Treatments for early NETs include somatostatin analogue
subcutaneous injections, such as Sandostatin LAR(R) (octreotide)
and Somatuline Depot(R) (lanreotide) and Afinitor(R) for
well-differentiated, non-functional gastrointestinal and lung NETs.
Somatostatin analogues help alleviate symptoms and slow NET growth,
but have limited tumor reduction efficacy and are approved and
reimbursed in China. Afinitor(R) is not approved for use in
gastrointestinal and lung NETs in China.
Advanced NETs are generally poorly differentiated, looking less
like healthy cells, growing more quickly with generally a higher
Mitotic count and Ki-67 index. Approved targeted therapies outside
China, for patients with advanced NETs include Sutent(R) and
Afinitor(R) , both oral treatments, for pancreatic NET and
Lutathera(R) (177 Lu-Dotatate), a somatostatin receptor targeting
radiotherapy, is approved for somatostatin receptor-positive GEP
NETs. Lutathera(R) is a subcutaneous injection, which has a
half-life of 72 hours and requires radiopharmaceutical-qualified
physicians to administer the drug, making it impractical today for
the China market. In China, Sutent(R) and Afinitor(R) are only
approved for pancreatic NET and no targeted therapies are approved
for the approximately 80% of NET patients with non-pancreatic
NET.
Phase III study of surufatinib monotherapy in non-pancreatic NET
(SANET-ep) (NCT02588170) - In 2015, we initiated the SANET-ep
study, which is a Phase III study in China in patients with low- or
intermediate-grade advanced extra-pancreatic NET. In this study,
patients are randomized at a 2:1 ratio to receive either an oral
dose of 300 mg of surufatinib or placebo once daily on a 28-day
treatment cycle. The primary endpoint is PFS, with secondary
endpoints including ORR, DCR, duration of response, OS, safety and
tolerability.
In June 2019, at the interim analysis of our SANET-ep study, the
IDMC confirmed that the trial met its primary endpoint of
superiority in PFS as compared to placebo. As a result, the study
was un-blinded a year ahead of schedule, and preparations for an
NDA submission are now underway for this indication in China.
We believe the benefit of surufatinib as a monotherapy to
patients with extra-pancreatic NET in China could be significant as
compared to the minimal treatment alternatives currently available
to them. We expect to submit the results of this trial for
publication or presentation at a scientific conference in late
2019.
Phase III study of surufatinib monotherapy in pancreatic NET
(SANET-p) (NCT02589821) - In 2016, we initiated the SANET-p study,
which is a Phase III study in China in patients with low- or
intermediate-grade, advanced pancreatic NET. In this study,
patients are randomized at a 2:1 ratio to receive either an oral
dose of 300 mg of surufatinib or a placebo once daily on a 28-day
treatment cycle. The primary endpoint is PFS, with secondary
endpoints including ORR, DCR, duration of response, OS, safety and
tolerability. We expect to conduct a final interim analysis in
early 2020.
Global development of surufatinib in NET - Surufatinib is
currently in a Phase Ib study in the U.S. in pancreatic NET
patients that are refractory to Sutent(R) and Afinitor(R) .
Planning is currently underway for a global Phase II/III study that
is expected to initiate during H1 2020.
Surufatinib - Biliary Tract Cancer (BTC):
Phase Ib/IIa study of surufatinib monotherapy in BTC
(NCT02966821) - In early 2017, we began a Phase Ib/IIa
proof-of-concept study in patients with BTC, a heterogeneous group
of rare malignancies arising from the biliary tract epithelia. This
is a major unmet medical need for patients who have progressed on
first-line chemotherapy, and there is currently no standard of care
for these patients.
Phase IIb/III study of surufatinib monotherapy in second line
BTC (NCT03873532) - In March 2019, based on our preliminary Phase
Ib/IIa data we initiated a registration-intent Phase IIb/III study
comparing surufatinib with capecitabine in patients with advanced
BTC whose disease progressed on first-line chemotherapy. The study
is a randomized, open-label, active-control, multi-center, study
investigating the effects of surufatinib versus the chemotherapy
agent capecitabine, as a second-line therapy in patients with
unresectable or metastatic BTC. The primary endpoint is OS.
Secondary outcomes include PFS, ORR, DCR, duration of response,
quality of life, tumor biomarkers, and safety.
Surufatinib - Combinations with Checkpoint Inhibitors:
In November 2018, we entered into collaboration agreements to
evaluate the safety, tolerability and efficacy of surufatinib in
combination with checkpoint inhibitors. These include a global
collaboration to evaluate the combination of surufatinib with
Junshi's Tuoyi(R) (toripalimab, JS001), a PD-1 monoclonal antibody
approved in China in late 2018. A Phase I safety run-in study of
surufatinib in combination with Tuoyi(R) in China is enrolling.
HMPL-523
HMPL-523 is an oral inhibitor targeting Syk, a key protein
involved in B-cell signaling. We currently retain all rights to
HMPL-523 worldwide. The table below shows a summary of the clinical
studies for HMPL-523.
Treatment Name, Line, Patient Focus Sites Phase Status/Plan NCT #
==================== =============================== ========= ===== =========== ===========
HMPL-523 monotherapy Indolent non-Hodgkin's lymphoma Australia Ib Enrolling NCT02503033
==================== =============================== ========= ===== =========== ===========
HMPL-523 monotherapy Indolent non-Hodgkin's lymphoma US/EU I Enrolling NCT03779113
==================== =============================== ========= ===== =========== ===========
HMPL-523 monotherapy Multiple sub-types of B-cell China I/Ib Enrolling NCT02857998
malignancies
==================== =============================== ========= ===== =========== ===========
HMPL-523 and Acute myeloid leukemia China I Enrolling NCT03483948
Vidaza(R)
==================== =============================== ========= ===== =========== ===========
HMPL-523 monotherapy Immune thrombocytopenia China I/Ib Enrolling NCT03951623
purpura
==================== =============================== ========= ===== =========== ===========
Phase Ib studies of HMPL-523 in indolent non-Hodgkin's lymphoma
and multiple subtypes of B cell malignancies
(NCT02503033/NCT02857998) - In 2016 and 2017, we initiated Phase I
studies of HMPL-523 in hematological cancer in Australia and China
respectively which to-date in dose escalation and expansion have
enrolled over 150 non-Hodgkin's lymphoma patients. Since early
2018, we have been increasing the number of active clinical sites,
in Australia and China to support a large dose expansion program in
a broad range of hematological cancers. We intend to use safety and
efficacy data from these Phase I/Ib dose escalation/expansion
studies in B-cell malignancies to guide the registration strategy
in China during late 2019.
Phase I study of HMPL-523 in indolent non-Hodgkin's lymphoma
(NCT03779113) - Our IND applications for HMPL-523 were cleared in
the U.S. in mid-2018 and Europe in early-2019, multiple sites are
now initiated and patient screening is underway. We anticipate
treatment of our first indolent non-Hodgkin's lymphoma patients, in
this Phase I dose escalation study, in the U.S. and Europe in the
second half of 2019.
Phase I study of HMPL-523 in combination with Vidaza(R) in acute
myeloid leukemia (NCT03483948) - In October 2018, we initiated a
Phase I study of HMPL-523 in combination with Vidaza(R)
(azacitidine), an approved hypomethylating agent, in elderly
patients with acute myeloid leukemia in China. This is a Phase I,
open-label, multicenter study to evaluate the safety,
pharmacokinetics ("PK") and preliminary efficacy of the combination
in previously untreated elderly patients with acute myeloid
leukemia. The primary outcome measure is safety with a secondary
endpoint of efficacy. The two-stage study will have a dose
escalation and dose expansion stage.
Phase I/Ib study of HMPL-523 in patients with immune
thrombocytopenia purpura ("ITP") - We are also considering
immunology applications for HMPL-523 including ITP, an autoimmune
disorder characterized by low platelet count and an increased
bleeding risk. Despite availability of several treatments with
differing mechanisms of action, a significant proportion of
patients develop resistance to treatment and are prone to relapse.
There is also a significant population of patients who have limited
sensitivity to currently available agents and are in need of a new
approach to treatment. A Phase I/Ib study in ITP in China is now
screening patients for enrollment.
HMPL-689
HMPL-689 is a novel, highly selective and potent small molecule
inhibitor targeting the isoform PI3K , a key component in the
B-cell receptor signaling pathway. We have designed HMPL-689 with
superior PI3K isoform selectivity than currently available agents.
HMPL-689's PK properties are favorable with good oral absorption,
moderate tissue distribution and low clearance in preclinical PK
studies. We also expect that HMPL-689 will have low risk of drug
accumulation and drug-to-drug interaction.
We currently retain all rights to HMPL-689 worldwide. The table
below shows a summary of the clinical studies for HMPL-689.
Treatment Name, Line, Patient Sites Phase Status/Plan NCT #
Focus
==================== ====================== ========= ===== =========== ===========
HMPL-689 monotherapy Healthy volunteers Australia I Completed NCT02631642
==================== ====================== ========= ===== =========== ===========
HMPL-689 monotherapy Indolent non-Hodgkin's US/EU I In planning NCT03786926
lymphoma
==================== ====================== ========= ===== =========== ===========
HMPL-689 monotherapy Indolent non-Hodgkin's China Ib Enrolling NCT03128164
lymphoma
==================== ====================== ========= ===== =========== ===========
In 2016, we completed a Phase I, first-in-human, dose escalation
study in healthy adult volunteers in Australia to evaluate the
pharmacokinetics and safety profile following single oral dosing
HMPL-689. Results were as expected with linear pharmacokinetics
properties and tolerable safety profile. In late 2017, we initiated
a Phase I dose escalation study in patients with hematologic
malignancies and have recently completed selection of a recommended
Phase II dose. We are now conducting a Phase Ib expansion in China;
and have also opened clinical sites in the U.S. and Europe in order
to start a Phase I study this year.
Epitinib (HMPL-813)
Epitinib is a potent and highly selective oral EGFR inhibitor
which has demonstrated brain penetration and efficacy in both
pre-clinical and clinical studies. Epitinib is designed to improve
blood-brain barrier penetration of the drug, allowing for high drug
exposure in the brain. We currently retain all rights to epitinib
worldwide. The table below shows a summary of the clinical studies
for epitinib.
Treatment Name, Line, Patient Focus Sites Phase Status/Plan NCT #
==================== ========================= ===== ===== =========== ===========
Epitinib monotherapy Glioblastoma China Ib/II Enrolling NCT03231501
==================== ========================= ===== ===== =========== ===========
Epitinib monotherapy EGFR-mutation NSCLC with China Ib Completed NCT02590952
brain metastasis
==================== ========================= ===== ===== =========== ===========
Glioblastoma: Glioblastoma is a very aggressive disease with
poor prognosis. There are currently no targeted therapies approved
for glioblastoma. EGFR gene amplification has been identified in
about half of glioblastoma patients, according to The Cancer Genome
Atlas Research Network, and hence is a potential therapeutic target
in glioblastoma. In March 2018, we initiated a Phase Ib/II,
multi-center, single-arm, open-label study to evaluate the efficacy
and safety of epitinib as a monotherapy in patients with EGFR gene
amplified, histologically confirmed glioblastoma. Enrollment is
ongoing.
HMPL-453
HMPL-453 is a highly selective and potent, small molecule that
targets FGFR 1/2/3, a sub-family of receptor tyrosine kinases. A
growing body of evidence has demonstrated the oncogenic potential
of FGFR aberrations in driving tumor growth, promoting
angiogenesis, and conferring resistance mechanisms to oncology
therapies. Targeting the FGF/FGFR signaling pathway has therefore
attracted attention from biopharmaceutical companies and has become
an important exploratory target for new anti-tumor target
therapies. We currently retain all rights to HMPL-453 worldwide.
The table below shows a summary of the clinical studies for
HMPL-453.
Treatment Name, Line, Patient Sites Phase Status/Plan NCT #
Focus
==================== =================== ===== ===== =========== ===========
HMPL-453 monotherapy Solid tumors China I Enrolling NCT03160833
==================== =================== ===== ===== =========== ===========
In June 2017, we initiated a Phase I clinical trial of HMPL-453
in China. This Phase I study is a multi-center, single-arm,
open-label, two-stage study to evaluate safety, tolerability,
pharmacokinetics and preliminary efficacy of HMPL-453 monotherapy
in patients with solid tumors harboring FGFR genetic alterations.
Enrollment is ongoing and planning for further development is
underway.
Theliatinib (HMPL-309)
Theliatinib is a novel small molecule EGFR inhibitor. Tumors
with wild-type EGFR activation, for instance, through gene
amplification or protein over-expression, are less sensitive to
EGFR TKIs such as Iressa(R) and Tarceva(R) due to sub-optimal
binding affinity. Theliatinib was designed with strong affinity to
the wild-type EGFR kinase and has demonstrated five to ten times
the potency than Tarceva(R) in pre-clinical trials. As a result, we
believe that theliatinib could potentially be more effective than
existing EGFR TKI products and benefit patients with tumor types
with high incidence of wild-type EGFR activation.
We currently retain all rights to theliatinib worldwide. Phase
I/Ib studies of theliatinib are complete and we are now looking at
alternative uses of theliatinib and could consider the potential
for use in combinations with immunotherapy.
DISCOVERY RESEARCH & PRECLINICAL DEVELOPMENT
We continue to create differentiated novel oncology and
immunology treatments with global potential.
These novel drug candidates reflect our core R&D philosophy
in treating cancer and immunological diseases through multiple
modalities and mechanisms. These include furthering pre-clinical
programs for therapies addressing aberrant genetic drivers,
inactivated T-cell response, and insufficient T-cell response. The
aim of our in-house discovery organization is to submit a novel
drug candidate for clinical development each year or so.
Importantly, we will continue to design drug candidates with
profiles that enable them to be used in innovative combinations
with other selective inhibitors, chemotherapy agents and
immunotherapies. Such combination therapies enable treatment of
cancer via multiple pathways and modalities simultaneously, which
has the potential to significantly improve treatment outcomes.
In June 2019 we submitted an IND application to the NMPA for
HMPL-306, a novel small molecule dual-inhibitor of IDH 1 and 2
enzymes. IDH1 and IDH2 mutations have been implicated as drivers of
certain hematological malignancies, gliomas and solid tumors,
particularly amongst acute myeloid leukemia (AML) patients.
COMMERCIAL Platform
Our Commercial Platform is a large-scale, high-performance drug
marketing and distribution platform covering over 330 cities and
towns in China with approximately 3,300 sales personnel. It targets
multiple therapeutic areas with several household-name brands.
Built over the past 18 years, it is focused on two main business
areas.
First, our Prescription Drugs business is a higher-margin/profit
business operated through our joint ventures Hutchison Sinopharm
and SHPL, in which we nominate management and run the day-to-day
operations. Aspects of our Prescription Drugs business form a core
strategic platform that we plan to use to launch our Innovation
Platform drugs once approved in China. Second, our Consumer Health
business is a profitable and cash flow generating business
primarily selling market-leading, household-name over-the-counter
("OTC") pharmaceutical products through our non-consolidated joint
venture HBYS.
During the first half of 2019, global macroeconomic factors
including, but not limited to, the trade discussions between the
United States and China contributed to a 6% depreciation in the
value of the RMB against the U.S. dollar versus H1 2018. As a
result, in addition to reporting changes in performance in our
normal U.S. dollar method, we also report changes in performance at
constant exchange rate (CER) which is a non-GAAP measure. Please
refer to "Use of Non-GAAP Financial Measures and Reconciliation"
below for further information relevant to the interpretation of
these financial measures and reconciliations of these financial
measures to the most comparable GAAP measures.
During the first half of 2019, the Commercial Platform delivered
continued solid growth in sales and net income growth on a CER
basis. Consolidated sales of our Commercial Platform's subsidiaries
grew by 2% (7% at CER) to $90.2 million (H1-18: $88.6m). The sales
of our Commercial Platform's non-consolidated joint ventures, SHPL
and HBYS, also grew by 2% (8% at CER) to $276.9 million (H1-18:
$271.7m). This resulted in consolidated net income attributable to
Chi-Med from our Commercial Platform up 3% (9% at CER) to $27.7
million (H1-18: $26.9m).
PRESCRIPTION DRUGS BUSINESS:
In H1 2019, consolidated sales of our Prescription Drugs
subsidiaries increased by 7% (13% at CER) to $72.6 million (H1-18:
$68.0m), despite the halt of the Seroquel(R) business as detailed
below. The consolidated net income attributable to Chi-Med from our
Prescription Drugs business was up 5% (11% at CER) to $21.8 million
(H1-18: $20.8m). The Prescription Drugs business represented 79% of
our overall Commercial Platform net income in H1 2019 (H1-18:
77%).
SHPL: Our own-brand Prescription Drugs business, operated
through our non-consolidated joint venture SHPL, is a
well-established large-scale business. In H1 2019, SHPL delivered
sales growth of 4% (10% at CER) at $158.9 million (H1-18: $152.7m),
as a result of both volume and price growth on SXBX pill.
SXBX pill: SHPL's main product is SXBX pill, an oral vasodilator
and pro-angiogenesis prescription therapy approved to treat
coronary artery disease, which includes stable/unstable angina,
myocardial infarction and sudden cardiac death. There are over one
million deaths due to coronary artery disease per year in China,
with this number set to rise due to an aging population with high
levels of smoking (28% of adults), increasing levels of obesity
(30% of adults are overweight) and hypertension (25% of adults).
SXBX pill is the third largest botanical prescription drug in this
indication in China, with market share in 2018 of 17.0% (2017:
15.4%) nationally and 48.0% (2017: 47.0%) in Shanghai.
Sales of SXBX pill have grown more than twenty-fold since 2001
due to continued geographical expansion of sales coverage,
including 9% (15% at CER) to $141.0 million in H1 2019 (H1-18:
$129.8m).
SXBX pill is protected by a formulation patent that expires in
2029 and is one of less than two dozen proprietary prescription
drugs represented on China's National Essential Medicines List,
which means that all Chinese state-owned health care institutions
are required to carry the drug. SXBX pill is a low-cost drug, fully
reimbursed in all provinces in China, listed on China's Low Price
Drug List with an average daily cost of RMB4.52 (H1-18: RMB4.17),
or approximately $0.67.
In January 2019, SHPL was awarded the 2018 State Scientific and
Technological Progress Award ("SSTPA") - Second Prize, which was
presented by President Xi Jinping, Premier Li Keqiang and other
state leaders of the PRC at the National Science and Technology
Awards Ceremony. The award was given for a study, conducted by SHPL
and several academic and medical institutions in China, on the
basis of the substance, mechanism of action, clinical evidence and
production chain control of SXBX pill. This SHPL award was one of
only two such SSTPA awards given this year to studies in the
botanical drug industry.
The SHPL operation is large-scale in both the commercial and
manufacturing areas. The commercial team now has about 2,400
medical sales representatives which allows for the promotion and
scientific detailing of our prescription drug products not just in
hospitals in provincial capitals and medium-sized cities, but also
in the majority of county-level hospitals in China.
SHPL's GMP-certified factory located 40 kilometers south of
Shanghai in Fengpu district holds 74 drug product manufacturing
licenses and is operated by about 540 manufacturing staff. This
factory, opened in 2017, has approximately tripled SHPL's capacity
and therefore positions us well for continued long-term growth.
Concor(R) : Concor(R) (Bisoprolol tablets) is a cardiac
beta1-receptor blocker, relieving hypertension and reducing high
blood pressure. Concor(R) is the number two beta-blocker in China
in 2018 with an approximately 24% (2017: 18%) national market share
in China's beta-blocker drug market and 63% of China's generic
bisoprolol market. In early 2019, we re-structured our
collaboration agreement with Merck Serono on Concor(R) , making
territorial adjustments and expanding SHPL operations on Concor(R)
into nine provinces in China (2018: six), markets that contain
about 600 million people.
Hutchison Sinopharm: Our Prescription Drugs commercial services
business, which in addition to commercializing certain of our own
products, provides distribution and marketing services to
third-party pharmaceutical companies in China. In H1 2019,
Hutchison Sinopharm sales grew by 7% (13% at CER) to $72.6 million
(H1-18: $68.0m) as a result of broad scale expansion which was
partially offset by the halt of Seroquel(R) commercial
operations.
Hutchison Sinopharm has a dedicated team of over 200 commercial
staff focused on three key areas of operation.
Firstly, a commercial team that markets over 700 third-party
prescription drug products directly to over 360 public and private
hospitals in the Shanghai region and through a network of 50
distributors to cover all other provinces in China.
Second, a commercial team that markets Chi-Med's own
science-based infant nutrition products in over 8,000 outlets in
China and through a Customer Relationship Management network with
over 23,000 promoters and over 200,000 members.
Third, during the second half of 2018 we began establishing an
oncology commercial organization within Hutchison Sinopharm, which
is cross-charged in full to the Innovation Platform. The oncology
team, which currently has about 60 dedicated staff covering 25
provinces in China, is focused on medical affairs activities to
support enrollment of our Innovation Platform clinical studies in
China as well as preparation for the potential upcoming commercial
launch of surufatinib late next year. Given the strategic
importance of this activity, we are now preparing to move the
oncology commercial organization into our 99.8%-owned Innovation
Platform.
Seroquel(R) update: Seroquel(R) (quetiapine tablets) is an
anti-psychotic therapy approved for bi-polar disorder and
schizophrenia. Since early 2015, Hutchison Sinopharm has been the
exclusive marketing agent for Seroquel(R) tablets in China. In June
2018, AstraZeneca sold and licensed its rights to Seroquel(R) to
Luye Pharma Group, Ltd., including its rights in China. The terms
of our agreement with AstraZeneca were assigned to Luye Pharma Hong
Kong Ltd. ("Luye HK"). In May 2019, we received a notice from Luye
HK purporting to terminate our agreement. We believe that Luye HK
has no basis for termination and intend to vigorously enforce our
rights under the current agreement. During 2018 and the first half
of 2019, net income from our Seroquel(R) business represented
approximately 4.0% ($1.7m) and 1.3% ($0.4m) respectively of the net
income attributable to Chi-Med from our Commercial Platform.
CONSUMER HEALTH BUSINESS:
In H1 2019, sales of our Consumer Health subsidiaries decreased
by 15% (13% at CER) to $17.6 million (H1-18: $20.6m) due primarily
to rationalization of certain low contribution products. The
consolidated net income attributable to Chi-Med from our Consumer
Health business was down 4% (up 2% at CER) to $5.9 million (H1-18:
$6.1m). The Consumer Health business represented 21% of our overall
Commercial Platform net income in H1 2019 (H1-18: 23%).
HBYS: Our primarily OTC business operated through our
non-consolidated joint venture, HBYS, focuses on the manufacture,
marketing and distribution of OTC and certain prescription
pharmaceutical products. In H1 2019, HBYS sales fell 1% (up 5% at
CER) to $118.0 million (H1-18: $119.0m), as a result of a decrease
in sales of Fu Fang Dan Shen ("FFDS") due to heightened competitive
activity, offset by the increase of sales of our second wave
products.
Its Bai Yun Shan brand is a market-leading, household name,
established over 40 years ago, and is known by the majority of
Chinese consumers. In addition to about 1,000 manufacturing staff
in Guangdong and Anhui and 185 drug product licenses, HBYS has a
commercial team of about 900 sales staff that covers the national
retail pharmacy channel in China.
FFDS tablets and Banlangen granules: FFDS tablets (angina) and
Banlangen granules (anti-viral cold/flu), the two main products of
HBYS, are generic OTC drugs with leading national market share in
2018 in China of 38% (2017: 38%) and 54% (2017: 53%), respectively.
In H1 2019, the combined sales of these products decreased by 6%
(0% at CER) at $66.4 million (H1-18: $70.7m). Banlangen sales were
down 1% (up 6% at CER) to $37.7 million (H1-18: $37.9m) as a result
of a similar flu season to early 2018. FFDS sales were down 13% (7%
at CER) to $28.7 million (H1-18: $32.8m) due to heightened
competitive activity.
Given the relative market maturity, and highly competitive
environment, for FFDS and Banlangen, HBYS has invested significant
resources in recent years into building out a second wave of
products. These products, including Nao Xin Qing tablets
(cerebrovascular diseases) and Kou Yan Qing granules
(periodontitis), made solid progress during the first half of 2019
growing 20% (28% at CER) to $33.5 million (H1-18: $27.8m).
HBYS property update: HBYS's vacant Plot 2 (26,700 sqm.) in
Guangzhou has been listed for sale as part of the Guangzhou
municipal government's urban redevelopment scheme plan for three
years. We expect the auction value for Plot 2 to be well over $100
million of which 40 to 50% would be paid to HBYS as compensation
for return of the land use rights. In addition, the move away from
HBYS's larger Plot 1 (59,400 sqm.) will be contingent on how the
Bozhou factory develops, but, when auctioned, we anticipate that
based on recent precedent land transactions, Plot 1 could bring
HBYS compensation per square meter comparable to Plot 2.
Hutchison Healthcare Limited ("HHL") and Hutchison Hain Organic
Holdings Limited ("HHOH"): HHL, HHOH and other minor entities are
subsidiaries involved in the commercialization of health-related
consumer products. Sales of such products in H1 2019 decreased by
15% (13% at CER) to $17.6 million (H1-18: $20.6m) resulting from a
rationalization of certain low contribution products primarily
under HHOH.
Commercial Platform dividends:
The profits of the Commercial Platform continue to pass on to
the Chi-Med Group through dividend payments primarily from our
non-consolidated joint ventures, SHPL and HBYS. Dividends of $18.2
million (H1-18: $23.5m) were paid from these joint ventures to the
Chi-Med Group level during the first half of 2019. Net income from
SHPL and HBYS have totaled over $600 million since 2005, of which
$423 million has been declared in dividends to Chi-Med and its
partners, with the balance retained by the joint ventures as cash
or used primarily to fund factory upgrades and expansion. As of
June 30, 2019, SHPL and HBYS held in aggregate $47.3 million in
cash and cash equivalents, with no outstanding bank borrowings.
Christian Hogg
Chief Executive Officer
July 30, 2019
Use of Non-GAAP Financial Measures and Reconciliation
In addition to financial information prepared in accordance with
U.S. GAAP, this announcement also contains certain non-GAAP
financial measures based on management's view of performance
including:
-- Adjusted R&D expenses;
-- Adjusted Group net cash flows and adjusted Group net cash
flows excluding financing activities; and
-- CER.
Management uses such measures internally for planning and
forecasting purposes and to measure the Chi-Med Group's overall
performance. We believe these adjusted financial measures provide
useful and meaningful information to us and investors because they
enhance investors' understanding of the continuing operating
performance of our business and facilitate the comparison of
performance between past and future periods. These adjusted
financial measures are non-GAAP measures and should be considered
in addition to, but not as a substitute for, the information
prepared in accordance with U.S. GAAP. Other companies may define
these measures in different ways.
Adjusted R&D expenses: We exclude the impact of the revenue
received from external customers and cost of goods of our
Innovation Platform, which is reinvested into our clinical trials,
to derive our adjusted R&D expenses. Revenue received from
external customers of our Innovation Platform consists of milestone
and other payments from our collaboration partners. The variability
of such payments makes the identification of trends in our ongoing
R&D activities more difficult. We believe the presentation of
adjusted R&D expenses provides useful and meaningful
information about our ongoing R&D activities by enhancing
investors' understanding of the scope of our normal, recurring
operating R&D expenses.
Adjusted Group net cash flows and adjusted Group net cash flows
excluding financing activities: We include the change in short-term
investments for the period to the change in cash and cash
equivalents for the period to derive our adjusted Group net cash
flows, and exclude the net cash (used in)/generated from financing
activities for the period to derive our adjusted Group net cash
flows excluding financing activities. We believe the presentation
of adjusted Group net cash flows and adjusted Group net cash flows
excluding financing activities provides useful and meaningful
information about the use of our cash resources.
CER: We remove the effects of currency movements from
period-to-period comparisons by retranslating the current period's
performance at previous period's foreign currency exchange rates.
Because we have significant operations in China, the RMB to U.S.
dollar exchange rates used for translation may have a significant
effect on our reported results. We believe the presentation at CER
provides useful and meaningful information because it facilitates
period-to-period comparisons of our results and increases the
transparency of our underlying performance.
Reconciliation of GAAP to adjusted R&D expenses:
$'millions Six Months Six Months
Ended June Ended June
30, 2019 30, 2018
------------------------------------------------- ----------- -----------
Segment operating loss - Innovation Platform (63.9) (53.1)
Less: Segment revenue from external customers
- Innovation Platform (12.0) (13.6)
Add: Cost of goods - third parties 1.4 -
------------------------------------------------- ----------- -----------
Adjusted R&D expenses (74.5) (66.7)
------------------------------------------------- ----------- -----------
Reconciliation of GAAP change in cash and cash equivalents and
short-term investments to Adjusted Group net cash flows and
Adjusted Group net cash flows excluding financing activities:
$'millions H1 2019 2019 Current 2019 Previous
Guidance Guidance
---------------------------------------------- ------- ------------ -------------
Cash and cash equivalents and short-term
investments at end of period 237.3 180-210* 150-180*
Less: Cash and cash equivalents and
short-term investments at beginning
of year (301.0) (300) (300)
Adjusted Group net cash flows (63.7) (90)-(120) (120)-(150)
Add: Net cash used in financing activities 29.5 -* -*
for the period
---------------------------------------------- ------- ------------ -------------
Adjusted Group net cash flows excluding
financing activities (34.2) (90)-(120) (120)-(150)
---------------------------------------------- ------- ------------ -------------
* For the purposes of this reconciliation, 2019 guidance for net
cash used in or generated from financing activities for the year is
not provided and as such, cash and cash equivalents and short-term
investments at the end of year excludes the effect of any net cash
used in or generated from financing activities for the year.
Reconciliation of GAAP sales and net income attributable to
Chi-Med-Commercial Platform to CER:
$'millions (except Six Months
%) Ended Growth Amount Growth %
---------------------- -------------- -------------------------- -----------------------------------
June June Actual Exchange
30, 30, Exchange growth CER growth effect
2019 2018 Actual CER effect % % %
---------------------- ------ ------ ------- ------ --------- -------- ----------- ------------
Consolidated
sales
Commercial Platform 90.2 88.6 1.6 6.4 (4.8) 2% 7% -5%
- Prescription
Drugs 72.6 68.0 4.6 9.1 (4.5) 7% 13% -6%
- Consumer Health 17.6 20.6 (3.0) (2.7) (0.3) -15% -13% -2%
Non-consolidated
joint venture
sales 276.9 271.7 5.2 22.3 (17.1) 2% 8% -6%
- SHPL 158.9 152.7 6.2 15.8 (9.6) 4% 10% -6%
- HBYS 118.0 119.0 (1.0) 6.5 (7.5) -1% 5% -6%
Consolidated net income
attributable to Chi-Med
Commercial Platform 27.7 26.9 0.8 2.4 (1.6) 3% 9% -6%
- Prescription
Drugs 21.8 20.8 1.0 2.3 (1.3) 5% 11% -6%
- Consumer Health 5.9 6.1 (0.2) 0.1 (0.3) -4% 2% -6%
Sales of Key
Products
- SXBX pill 141.0 129.8 11.2 19.7 (8.5) 9% 15% -6%
- FFDS and Banlangen 66.4 70.7 (4.3) (0.2) (4.1) -6% 0% -6%
- FFDS 28.7 32.8 (4.1) (2.3) (1.8) -13% -7% -6%
- Banlangen 37.7 37.9 (0.2) 2.1 (2.3) -1% 6% -7%
- Nao Xin Qing
and Kou Yan Qing 33.5 27.8 5.7 7.7 (2.0) 20% 28% -8%
INTERIM UNAUDITED CONDENSED CONSOLIDATED FINANCIAL
STATEMENTS
Hutchison China MediTech Limited
Condensed Consolidated Balance Sheets
(in US$'000, except share data)
June 30, December 31,
Note 2019 2018
----- ------------ -------------
(Unaudited)
Assets
Current assets
Cash and cash equivalents 3 83,360 86,036
Short-term investments 4 153,928 214,915
Accounts receivable-third parties 5 42,758 40,176
Inventories 6 14,223 12,309
Other current assets 15,227 17,105
------------ -------------
Total current assets 309,496 370,541
Property, plant and equipment 17,669 16,616
Right-of-use assets 7 6,792 -
Investments in equity investees 8 146,977 138,318
Deferred issuance costs 7,506 -
Other assets 6,774 6,643
------------ -------------
Total assets 495,214 532,118
============ =============
Liabilities and shareholders' equity
Current liabilities
Accounts payable 9 26,145 25,625
Other payables, accruals and advance receipts 10 75,567 56,327
Lease liabilities 7 3,529 -
Other current liabilities 5,364 3,527
------------ -------------
Total current liabilities 110,605 85,479
Lease liabilities 7 3,714 -
Long-term bank borrowings 11 - 26,739
Other liabilities 7,858 7,645
------------ -------------
Total liabilities 122,177 119,863
Commitments and contingencies 12
Company's shareholders' equity
Ordinary shares; $0.10 par value; 1,500,000,000 shares authorized; 666,577,450
and 666,577,450
shares issued at June 30, 2019 and December 31, 2018 respectively 13 66,658 66,658
Additional paid-in capital 510,699 505,585
Accumulated losses (229,067) (183,004)
Accumulated other comprehensive loss (400) (243)
------------ -------------
Total Company's shareholders' equity 347,890 388,996
Non-controlling interests 25,147 23,259
------------ -------------
Total shareholders' equity 373,037 412,255
------------ -------------
Total liabilities and shareholders' equity 495,214 532,118
============ =============
The accompanying notes are an integral part of these interim
unaudited condensed consolidated financial statements.
Hutchison China MediTech Limited
Condensed Consolidated Statements of Operations
(Unaudited, in US$'000, except share and per share data)
Six Months Ended
June 30,
--------------------------
Note 2019 2018
------ ------------ ------------
Revenues
Goods -third parties 86,858 79,463
-related parties 17(i) 3,732 3,449
Services -commercialization-third parties 2,584 5,653
-collaboration research and development-third parties 7,056 8,548
-research and development-related parties 17(i) 252 5,076
Other collaboration revenue-royalties-third parties 1,715 -
------------ ------------
Total revenues 15 102,197 102,189
------------ ------------
Operating expenses
Costs of goods-third parties (74,051) (65,422)
Costs of goods-related parties (2,610) (2,455)
Costs of services-commercialization-third parties (1,929) (4,001)
Research and development expenses 16 (69,287) (60,053)
Selling expenses (7,501) (9,392)
Administrative expenses (18,830) (14,549)
------------ ------------
Total operating expenses (174,208) (155,872)
------------ ------------
Loss from operations (72,011) (53,683)
Other income, net of other expenses 3,710 3,188
------------ ------------
Loss before income taxes and equity in earnings of equity investees (68,301) (50,495)
Income tax expense 18 (2,462) (2,680)
Equity in earnings of equity investees, net of tax 8 27,308 23,050
------------ ------------
Net loss (43,455) (30,125)
Less: Net income attributable to non-controlling interests (1,914) (2,566)
------------ ------------
Net loss attributable to the Company (45,369) (32,691)
============ ============
Losses per share attributable to the Company-basic and diluted (US$ per share) 19 (0.07) (0.05)
Number of shares used in per share calculation-basic and diluted 19 665,553,637 663,894,540
Note: The losses per share attributable to the Company-basic and
diluted presented were adjusted retroactively for each of the six
months ended June 30, 2019 and 2018 to take into account the share
split approved by ordinary resolution at the Extraordinary General
Meeting of the Company held on May 29, 2019, pursuant to which each
ordinary share was subdivided into 10 ordinary shares with effect
from May 30, 2019.
The accompanying notes are an integral part of these interim
unaudited condensed consolidated financial statements.
Hutchison China MediTech Limited
Condensed Consolidated Statements of Comprehensive Loss
(Unaudited, in US$'000)
Six Months Ended
June 30,
--------------------
2019 2018
--------- ---------
Net loss (43,455) (30,125)
Other comprehensive income
Foreign currency translation (loss)/gain (179) 3,445
--------- ---------
Total comprehensive loss (43,634) (26,680)
Less: Comprehensive income attributable to non-controlling interests (1,892) (2,870)
--------- ---------
Total comprehensive loss attributable to the Company (45,526) (29,550)
========= =========
The accompanying notes are an integral part of these interim
unaudited condensed consolidated financial statements.
Hutchison China MediTech Limited
Condensed Consolidated Statements of Changes in Shareholders'
Equity
(Unaudited, in US$'000, except share data in '000)
Accumulated Total
Ordinary Ordinary Additional Other Company's Non- Total
Shares Shares Paid-in Accumulated Comprehensive Shareholders' controlling Shareholders'
Number Value Capital Losses Income/(Loss) Equity Interests Equity
--------- --------- ----------- ------------ -------------- -------------- ------------ --------------
As at January
1, 2018 664,470 66,447 496,960 (108,184) 5,430 460,653 23,230 483,883
Net
(loss)/income - - - (32,691) - (32,691) 2,566 (30,125)
Issuances in
relation to
share option
exercises 856 86 634 - - 720 - 720
Share-based
compensation
Share
options - - 2,784 - - 2,784 7 2,791
Long-term
incentive
plan
("LTIP") - - 2,575 - - 2,575 7 2,582
--------- --------- ----------- ------------ -------------- -------------- ------------ --------------
- - 5,359 - - 5,359 14 5,373
LTIP-treasury
shares
acquired and
held by
Trustee - - (5,451) - - (5,451) - (5,451)
Transfer
between
reserves - - 15 (15) - - - -
Foreign
currency
translation
adjustments - - - - 3,141 3,141 304 3,445
--------- --------- ----------- ------------ -------------- -------------- ------------ --------------
As at June 30,
2018 665,326 66,533 497,517 (140,890) 8,571 431,731 26,114 457,845
========= ========= =========== ============ ============== ============== ============ ==============
As at December
31, 2018 666,577 66,658 505,585 (183,004) (243) 388,996 23,259 412,255
Impact of
change in
accounting
policy (Note
2) - - - (655) - (655) (16) (671)
--------- --------- ----------- ------------ -------------- -------------- ------------ --------------
As at January
1, 2019 666,577 66,658 505,585 (183,659) (243) 388,341 23,243 411,584
Net
(loss)/income - - - (45,369) - (45,369) 1,914 (43,455)
Share-based
compensation
Share
options - - 4,118 - - 4,118 9 4,127
LTIP - - 1,303 - - 1,303 3 1,306
--------- --------- ----------- ------------ -------------- -------------- ------------ --------------
- - 5,421 - - 5,421 12 5,433
LTIP-treasury
shares
acquired and
held by
Trustee - - (346) - - (346) - (346)
Transfer
between
reserves - - 39 (39) - - - -
Foreign
currency
translation
adjustments - - - - (157) (157) (22) (179)
--------- --------- ----------- ------------ -------------- -------------- ------------ --------------
As at June 30,
2019 666,577 66,658 510,699 (229,067) (400) 347,890 25,147 373,037
========= ========= =========== ============ ============== ============== ============ ==============
The accompanying notes are an integral part of these interim
unaudited condensed consolidated financial statements.
Hutchison China MediTech Limited
Condensed Consolidated Statements of Cash Flows
(Unaudited, in US$'000)
Six Months Ended
June 30,
----------------------
Note 2019 2018
-------- ---------- ----------
Net cash used in operating activities 21 (30,045) (18,596)
---------- ----------
Investing activities
Purchases of property, plant and equipment (3,848) (2,079)
Deposits in short-term investments (329,102) (491,169)
Proceeds from short-term investments 390,089 517,035
Investment in an equity investee - (8,000)
---------- ----------
Net cash generated from investing activities 57,139 15,787
---------- ----------
Financing activities
Proceeds from issuance of ordinary shares 14(i) - 720
Purchases of treasury shares 14(ii) (346) (5,451)
Dividends paid to non-controlling shareholders of subsidiaries 17(iii) (1,282) -
Proceeds from bank borrowings 11 - 26,923
Repayment of bank borrowings 11 (26,923) (30,000)
Payment of issuance costs (964) (34)
---------- ----------
Net cash used in financing activities (29,515) (7,842)
---------- ----------
Net decrease in cash and cash equivalents (2,421) (10,651)
Effect of exchange rate changes on cash and cash equivalents (255) 715
---------- ----------
(2,676) (9,936)
Cash and cash equivalents
Cash and cash equivalents at beginning of period 86,036 85,265
---------- ----------
Cash and cash equivalents at end of period 83,360 75,329
========== ==========
The accompanying notes are an integral part of these interim
unaudited condensed consolidated financial statements.
Hutchison China MediTech Limited
Notes to the Interim Unaudited Condensed Consolidated Financial
Statements
1. Organization and Nature of Business
Hutchison China MediTech Limited (the "Company") and its
subsidiaries (together the "Group") are principally engaged in
researching, developing, manufacturing and selling pharmaceuticals
and healthcare products. The Group and its equity investees have
research and development facilities and manufacturing plants in the
People's Republic of China (the "PRC") and sell their products
mainly in the PRC and Hong Kong.
Liquidity
As at June 30, 2019, the Group had accumulated losses of
US$229,067,000 primarily due to its spending in drug research and
development ("Drug R&D") activities. The Group regularly
monitors current and expected liquidity requirements to ensure that
it maintains sufficient cash balances and adequate credit
facilities to meet its liquidity requirements in the short and long
term. As at June 30, 2019, the Group had cash and cash equivalents
of US$83,360,000, short-term investments of US$153,928,000 and
unutilized bank borrowing facilities of US$146,282,000. Short-term
investments comprised of bank deposits maturing over three months.
The Group's operating plan includes the continued receipt of
dividends from certain of its equity investees. Dividends received
from equity investees for the six months ended June 30, 2019 and
2018 were US$18,173,000 and US$23,526,000 respectively.
Based on the Group's operating plan, the existing cash and cash
equivalents, short-term investments and unutilized bank borrowing
facilities are considered to be sufficient to meet the cash
requirements to fund planned operations and other commitments for
at least the next twelve months (the look-forward period used).
2. Summary of Significant Accounting Policies
Principles of Consolidation and Basis of Presentation
The interim unaudited condensed consolidated financial
statements have been prepared in conformity with generally accepted
accounting principles in the United States of America ("U.S. GAAP")
for interim financial information. Accordingly, they do not include
all of the information and footnotes required by U.S. GAAP for
complete financial statements. The interim unaudited condensed
consolidated financial statements have been prepared on the same
basis as the annual audited consolidated financial statements,
except for the adoption of Accounting Standards Codification
("ASC") 842, Leases ("ASC 842") as described below. In the opinion
of management, all adjustments, consisting of normal recurring
adjustments necessary for the fair statement of results for the
periods presented, have been included. The results of operations of
any interim period are not necessarily indicative of the results of
operations for the full year or any other interim period.
The comparative year-end condensed balance sheet data was
derived from the annual audited consolidated financial statements,
but is condensed to the same degree as the interim condensed
balance sheet data.
The interim unaudited condensed consolidated financial
statements and related disclosures have been prepared with the
presumption that users have read or have access to the annual
audited consolidated financial statements for the preceding fiscal
year.
The preparation of interim unaudited condensed consolidated
financial statements in conformity with U.S. GAAP requires
management to make estimates and assumptions that affect the
reported amounts of assets and liabilities and the disclosure of
contingent assets and liabilities at the date of the interim
unaudited condensed consolidated financial statements and the
reported amounts of revenues and expenses during the reporting
period. Estimates are used in determining items such as useful
lives of property, plant and equipment, write-down of inventories,
allowance for doubtful accounts, share-based compensation,
impairments of long-lived assets, impairment of other intangible
asset and goodwill, income tax expenses, tax valuation allowances,
revenues and cost accruals from research and development projects.
Actual results could differ from those estimates.
Leases
Summary of impact of applying ASC 842
The Group applied ASC 842 to its various leases at the date of
initial application of January 1, 2019. As a result, the Group has
changed its accounting policy for leases as detailed below. The
core principle of ASC 842 is that a lessee should recognize the
assets and liabilities that arise from leases. Therefore, the Group
recognizes in the condensed consolidated balance sheets liabilities
to make lease payments (the lease liabilities) and right-of-use
assets representing its right to use the underlying assets for
their lease terms. The Group applied ASC 842 using the optional
transition method by recognizing the cumulative effect as an
adjustment to opening accumulated losses as at January 1, 2019. The
comparative information prior to January 1, 2019 has not been
adjusted and continues to be reported under ASC 840, Leases ("ASC
840").
The Group assessed lease agreements as at January 1, 2019 under
ASC 842, except for short-term leases. The Group elected the
short-term lease exception for leases with a term of 12 months or
less and recognizes lease expenses for such leases on a
straight-line basis over the lease term and does not recognize
right-of-use assets or lease liabilities accordingly. As a result
of this assessment, the Group recorded an aggregate US$0.7 million
in additional lease expenses as a cumulative adjustment to opening
accumulated losses upon adoption. Additionally, the Group
recognized right-of-use assets and lease liabilities of US$5.7
million and US$6.4 million respectively as at January 1, 2019.
The lease liabilities were measured at the present value of the
remaining lease payments, discounted using the lessees' incremental
borrowing rate as at January 1, 2019. The Group's weighted average
incremental borrowing rate applied on January 1, 2019 was 3.97% per
annum.
A reconciliation of the Group's reported operating lease
commitments as at December 31, 2018 and the Group's lease
liabilities recognized upon adoption of ASC 842 as at January 1,
2019 is as follows:
(in US$'000)
-------------
Operating lease commitments as at December 31,
2018 (note (a)) 8,835
Less: Leases not commenced as at January 1, 2019 (3,676)
Less: Short-term leases (5)
Add: Adjustment as a result of the treatment
for a termination option (note (b)) 1,409
Less: Discount under the lessees' incremental
borrowing rate as at January 1, 2019 (206)
-------------
Lease liabilities recognized as at January 1,
2019 6,357
=============
Notes:
(a) Future aggregate minimum payments under non-cancellable
operating leases under ASC 840 were as follows:
December 31,
2018
-------------
(in US$'000)
Not later than 1 year 3,026
Between 1 to 2 years 2,735
Between 2 to 3 years 1,056
Between 3 to 4 years 882
Between 4 to 5 years 810
Later than 5 years 326
-------------
Total minimum lease payments 8,835
=============
(b) The Group leases its corporate offices in Hong Kong through
a support service agreement with an indirect subsidiary of CK
Hutchison Holdings Limited ("CK Hutchison"), which is the Company's
ultimate holding company. The support service agreement may be
terminated by giving 3-month advance notice; therefore, there was
no lease commitment beyond the 3-month advance notice period as at
December 31, 2018. This termination option is not considered
probable of exercise for the purposes of applying ASC 842.
The Group recognized right-of-use assets as at January 1, 2019
measured at their carrying amounts as if ASC 842 had been applied
since their commencement dates, but discounted using the lessees'
incremental borrowing rate as at January 1, 2019.
Recognized right-of-use assets upon adoption were as
follows:
(in US$'000)
-------------
Offices 4,877
Factories 383
Others 487
-------------
5,747
=============
There were no adjustments to net cash generated from/(used in)
operating activities, investing activities or financing activities
in the condensed consolidated statement of cash flows.
In applying ASC 842 for the first time, the Group has used the
following practical expedients permitted by the standard: (i) no
reassessment of whether any expired or existing contracts are or
contain leases; (ii) no reassessment of the lease classification
for any expired or existing leases; (iii) the exclusion of initial
direct costs for the measurement of the right-of-use assets at the
date of initial application; and (iv) the use of hindsight in
determining the lease term where the contract contains options to
extend or terminate the lease.
Updated accounting policy-ASC 842
In an operating lease, a lessee obtains control of only the use
of the underlying asset, but not the underlying asset itself. An
operating lease is recognized as a right-of-use asset with a
corresponding liability at the date which the leased asset is
available for use by the Group. The Group recognizes an obligation
to make lease payments equal to the present value of the lease
payments over the lease term. The lease terms may include options
to extend or terminate the lease when it is reasonably certain that
the Group will exercise that option.
Lease liabilities include the net present value of the following
lease payments: (i) fixed payments; (ii) variable lease payments;
and (iii) payments of penalties for terminating the lease if the
lease term reflects the lessee exercising that option, if any.
Lease liabilities exclude the following payments that are generally
accounted for separately: (i) non-lease components, such as
maintenance and security service fees and value added tax, and (ii)
any payments that a lessee makes before the lease commencement
date. The lease payments are discounted using the interest rate
implicit in the lease or if that rate cannot be determined, the
lessee's incremental borrowing rate being the rate that the lessee
would have to pay to borrow the funds in its currency and
jurisdiction necessary to obtain an asset of similar value,
economic environment and terms and conditions.
An asset representing the right to use the underlying asset
during the lease term is recognized that consists of the initial
measurement of the operating lease liability, any lease payments
made to the lessor at or before the commencement date less any
lease incentives received, any initial direct cost incurred by the
Group and any restoration costs.
After commencement of the operating lease, the Group recognizes
lease expenses on a straight-line basis over the lease term. The
right-of-use asset is subsequently measured at cost less
accumulated amortization and any impairment provision. The
amortization of the right-of-use asset represents the difference
between the straight-line lease expense and the accretion of
interest on the lease liability each period. The interest amount is
used to accrete the lease liability and to amortize the
right-of-use asset. There is no amount recorded as interest
expense.
Payments associated with short-term leases are recognized as
lease expenses on a straight-line basis over the period of the
leases.
Subleases of right-of-use assets are accounted for similar to
other leases. As an intermediate lessor, the Group separately
accounts for the head-lease and sublease unless it is relieved of
its primary obligation under the head-lease. Sublease income is
recorded on a gross basis separate from the head-lease expenses. If
the total remaining lease cost on the head-lease is more than the
anticipated sublease income for the lease term, this is an
indicator that the carrying amount of the right-of-use asset
associated with the head-lease may not be recoverable, and the
right-of-use asset will be assessed for impairment.
3. Cash and Cash Equivalents
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Cash at bank and on hand 71,860 78,556
Bank deposits maturing in three months
or less (note (a)) 11,500 7,480
--------- ---------
83,360 86,036
========= =========
Denominated in:
US$ (note (b)) 59,459 58,291
RMB (note (b)) 19,443 23,254
UK Pound Sterling ("GBP") (note (b)) 122 331
Hong Kong dollar ("HK$") 4,336 4,160
--------- ---------
83,360 86,036
========= =========
Notes:
(a) The weighted average effective interest rate on bank
deposits for the six months ended June 30, 2019 and the year ended
December 31, 2018 was 2.47% per annum and 1.98% per annum
respectively (with maturity ranging from 5 to 35 days and 7 to 90
days respectively).
(b) Certain cash and bank balances denominated in RMB, US$ and
GBP were deposited with banks in the PRC. The conversion of these
balances into foreign currencies is subject to the rules and
regulations of foreign exchange control promulgated by the PRC
government.
4. Short-term Investments
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Bank deposits maturing over three months
(note)
Denominated in:
US$ 153,548 214,538
HK$ 380 377
--------- ---------
153,928 214,915
========= =========
Note: The weighted average effective interest rate on bank
deposits for the six months ended June 30, 2019 and the year ended
December 31, 2018 was 2.77% per annum and 2.18% per annum
respectively (with maturity ranging from 91 to 97 days and 91 to
100 days respectively).
5. Accounts Receivable-Third Parties
Accounts receivable from contracts with customers, net of
allowance for doubtful accounts, consisted of the following:
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Accounts receivable, gross 42,779 40,217
Allowance for doubtful accounts (21) (41)
--------- ---------
Accounts receivable, net 42,758 40,176
========= =========
Substantially all accounts receivable are denominated in RMB,
US$ and HK$ and are due within one year from the end of the
reporting periods. The carrying values of accounts receivable
approximate their fair values due to their short-term
maturities.
Movements on the allowance for doubtful accounts:
2019 2018
------ -------
(in US$'000)
As at January 1 41 258
Increase in allowance for doubtful accounts 14 279
Decrease in allowance due to subsequent
collection (34) (235)
Write-off - (1)
Exchange difference - 2
------ -------
As at June 30 21 303
====== =======
6. Inventories
Inventories, net of provision for excess and obsolete
inventories, consisted of the following:
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Raw materials 1,865 652
Finished goods 12,358 11,657
--------- ---------
14,223 12,309
========= =========
7. Leases
The Group leases various offices, factories and other assets.
Lease contracts are typically within a period of 1 to 5 years.
Leases consisted of the following:
June 30, 2019
--------------
(in US$'000)
Right-of-use assets
Offices (note (a)) 6,038
Factories 251
Others (note (b)) 503
--------------
Total right-of-use assets 6,792
==============
Lease liabilities-current 3,529
Lease liabilities-non-current 3,714
--------------
Total lease liabilities 7,243
==============
Notes:
(a) Includes (i) US$0.2 million right-of-use asset for offices
in the United States of America that is leased through July 2023
which includes an option to renew the lease up to an additional 3
years; and (ii) US$1.2 million right-of-use asset for corporate
offices in Hong Kong that is leased through May 2021 which includes
a termination option with 3 months advance notice. The renewal and
termination options were not recognized as part of the right-of-use
assets and lease liabilities.
(b) Includes US$0.4 million right-of-use asset for retail space
in the United Kingdom that is leased through May 2022 which the
Group has subleased through May 2022.
Lease activities are summarized as follows:
Six Months Ended
June 30, 2019
-----------------
(in US$'000)
Lease expenses:
Short-term leases with lease terms equal or
less than 12 months 38
Leases with lease terms greater than 12 months 1,655
-----------------
1,693
=================
Sublease rental income 61
=================
Cash paid on lease liabilities (1,782)
=================
Non-cash: Lease liabilities recognized from
obtaining right-of-use assets 2,453
=================
The weighted average remaining lease term and the weighted
average discount rate as at June 30, 2019 was 2.85 years and 4.20%
respectively.
Future lease payments are as follows:
June 30, 2019
--------------
(in US$'000)
Lease payments:
Not later than 1 year 3,764
Between 1 to 2 years 1,973
Between 2 to 3 years 862
Between 3 to 4 years 650
Between 4 to 5 years 457
--------------
Total lease payments (note) 7,706
Less: Discount factor (463)
--------------
Total lease liabilities 7,243
==============
Note: Excludes future lease payments on lease not commenced as
at June 30, 2019 in the aggregate amount of US$0.9 million.
8. Investments in Equity Investees
Investments in equity investees consisted of the following:
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Hutchison Whampoa Guangzhou Baiyunshan
Chinese Medicine Company Limited ("HBYS") 59,695 60,992
Shanghai Hutchison Pharmaceuticals Limited
("SHPL") 78,593 68,812
Nutrition Science Partners Limited ("NSPL") 8,150 8,102
Other 539 412
--------- ---------
146,977 138,318
========= =========
All of the equity investees are private companies and there are
no quoted market prices available for their shares.
Summarized financial information for the significant equity
investees HBYS, SHPL and NSPL is as follows:
(i) Summarized balance sheets
Commercial Platform Innovation Platform
-------------------------------------------------- ------------------------
Consumer Health Prescription Drugs Drug R&D
HBYS SHPL NSPL
------------------------ ------------------------ ------------------------
June 30, December 31, June 30, December 31, June 30, December 31,
2019 2018 2019 2018 2019 2018
--------- ------------- --------- ------------- --------- -------------
(in US$'000)
Current assets 126,654 116,020 138,493 124,512 16,698 17,320
Non-current assets 98,552 100,353 97,568 98,532 - -
Current liabilities (86,064) (73,974) (77,644) (84,357) (398) (1,117)
Non-current liabilities (16,874) (17,302) (7,077) (6,909) - -
--------- ------------- --------- ------------- --------- -------------
Net assets 122,268 125,097 151,340 131,778 16,300 16,203
Non-controlling interests (2,877) (3,113) - - - -
--------- ------------- --------- ------------- --------- -------------
119,391 121,984 151,340 131,778 16,300 16,203
========= ============= ========= ============= ========= =============
(ii) Summarized statements of operations
Commercial Platform Innovation Platform
------------------------------------------ ----------------------
Consumer Health Prescription Drugs Drug R&D
HBYS SHPL NSPL(note(a))
------------------- --------------------- ----------------------
Six Months Ended Six Months Ended Six Months Ended
June 30, June 30, June 30,
------------------- --------------------- ----------------------
2019 2018 2019 2018 2019 2018
--------- -------- ---------- --------- -------- ------------
(in US$'000)
Revenue 118,047 118,983 158,874 152,717 - -
========= ======== ========== ========= ======== ============
Gross profit 64,527 59,155 114,687 108,802 - -
========= ======== ========== ========= ======== ============
Interest income 81 37 289 407 134 43
========= ======== ========== ========= ======== ============
Finance cost (9) (135) - - - -
========= ======== ========== ========= ======== ============
Profit/(loss) before taxation 14,272 14,306 49,534 45,942 97 (4,818)
Income tax expense (note (b)) (2,286) (2,362) (7,479) (7,127) - -
--------- -------- ---------- --------- -------- ------------
Net income/(loss) 11,986 11,944 42,055 38,815 97 (4,818)
Non-controlling interests 223 39 - - - -
--------- -------- ---------- --------- -------- ------------
Net income/(loss) attributable to the
shareholders of equity investee 12,209 11,983 42,055 38,815 97 (4,818)
========= ======== ========== ========= ======== ============
Notes:
(a) NSPL did not have any activity for the six months ended June
30, 2019 and primarily incurred research and development expenses
during the six months ended June 30, 2018.
(b) The main entities within the HBYS and SHPL groups have been
granted the High and New Technology Enterprise ("HNTE") status.
Accordingly, the entities were eligible to use a preferential
income tax rate of 15% for the six months ended June 30, 2019 and
2018.
For the six months ended June 30, 2019 and 2018, other
immaterial equity investees had net income of approximately
US$255,000 and US$120,000 respectively.
(iii) Reconciliation of summarized financial information
Reconciliation of the summarized financial information presented
to the carrying amount of investments in equity investees is as
follows:
Innovation
Commercial Platform Platform(note)
------------------------------------------ ------------------
Consumer Health Prescription Drugs Drug R&D
HBYS SHPL NSPL
------------------- --------------------- ------------------
2019 2018 2019 2018 2019 2018
--------- -------- ---------- --------- -------- --------
(in US$'000)
Opening net assets after non-controlling interests as
at January 1 121,984 110,616 131,778 132,731 16,203 38,401
Impact of change in accounting policy (ASC 842) (19) - (2) - - -
Net income/(loss) attributable to the shareholders of
equity investee 12,209 11,983 42,055 38,815 97 (4,818)
Dividends declared (14,615) - (21,731) (31,538) - -
Other comprehensive (loss)/income (168) 1,693 (760) 2,339 - -
Investments - - - - - 16,000
--------- -------- ---------- --------- -------- --------
Closing net assets after non-controlling interests as
at June 30 119,391 124,292 151,340 142,347 16,300 49,583
========= ======== ========== ========= ======== ========
Group's share of net assets 59,695 62,146 75,670 71,173 8,150 24,792
Goodwill - - 2,923 3,103 - -
--------- -------- ---------- --------- -------- --------
Carrying amount of investments as at June 30 59,695 62,146 78,593 74,276 8,150 24,792
========= ======== ========== ========= ======== ========
Note: The Innovation Platform includes other immaterial equity
investees. As at June 30, 2019 and December 31, 2018, the aggregate
carrying amount of investments in NSPL and other immaterial equity
investees was approximately US$8,689,000 and US$8,514,000
respectively.
The equity investees had the following capital commitments:
June 30, 2019
--------------
(in US$'000)
Property, plant and equipment
Contracted but not provided for 1,750
==============
9. Accounts Payable
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Accounts payable-third parties 19,217 14,158
Accounts payable-non-controlling shareholders
of subsidiaries (Note 17(iv)) 4,132 4,960
Accounts payable-related party (Note 17(ii)) 2,796 6,507
--------- ---------
26,145 25,625
========= =========
Substantially all accounts payable are denominated in RMB and
US$ and due within one year from the end of the reporting period.
The carrying values of accounts payable approximate their fair
values due to their short-term maturities.
10. Other Payables, Accruals and Advance Receipts
Other payables, accruals and advance receipts consisted of the
following:
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Accrued salaries and benefits 9,602 8,715
Accrued research and development expenses 42,960 28,883
Accrued selling and marketing expenses 4,530 4,675
Accrued administrative and other general
expenses 7,751 6,181
Deferred government incentives 505 1,817
Deposits 1,296 1,230
Dividend payable to a non-controlling shareholder
of a subsidiary (Note 17(iv)) - 1,282
Accrued issuance costs 6,542 -
Others 2,381 3,544
--------- ---------
75,567 56,327
========= =========
11. Bank Borrowings
Bank borrowings consisted of the following:
December
June 30, 31,
2019 2018
---------- ---------
(in US$'000)
Non-current - 26,739
========== =========
The weighted average interest rate for outstanding bank
borrowings for the six months ended June 30, 2019 and the year
ended December 31, 2018 was 3.29% per annum and 2.79% per annum
respectively. The carrying amounts of the Group's bank borrowings
were denominated in HK$. The Group had fully repaid the bank
borrowings in June 2019 and there were no outstanding bank
borrowings as at June 30, 2019.
(i) 3-year term loan and 18-month revolving loan facilities
In November 2017, the Group through its subsidiary, entered into
facility agreements with a bank for the provision of unsecured
credit facilities in the aggregate amount of HK$400,000,000
(US$51,282,000). The credit facilities included (i) a
HK$210,000,000 (US$26,923,000) 3-year term loan facility and (ii) a
HK$190,000,000 (US$24,359,000) 18-month revolving loan facility.
The term loan bore interest at 1.50% over the Hong Kong Interbank
Offered Rate ("HIBOR") per annum and an upfront fee of HK$1,575,000
(US$202,000). The revolving loan facility bore interest at 1.25%
over HIBOR per annum. The term loan was drawn in May 2018 and was
fully repaid in June 2019. The revolving loan facility expired in
May 2019.
(ii) 2-year revolving loan facilities
In August 2018, the Group through its subsidiary, entered into
two separate facility agreements with banks for the provision of
unsecured credit facilities in the aggregate amount of
HK$507,000,000 (US$65,000,000). The first credit facility is a
HK$351,000,000 (US$45,000,000) revolving loan facility, with a term
of 2 years and an annual interest rate of 1.35% over HIBOR. The
second credit facility is a HK$156,000,000 (US$20,000,000)
revolving loan facility, with a term of 2 years and an annual
interest rate of 1.35% over HIBOR. These credit facilities are
guaranteed by the Company. As at June 30, 2019 and December 31,
2018, no amount has been drawn from either of the revolving loan
facilities.
In February 2017, the Group through its subsidiary, entered into
two separate facility agreements with the banks for the provision
of unsecured credit facilities in the aggregate amount of
HK$546,000,000 (US$70,000,000). The first credit facility included
(i) a HK$156,000,000 (US$20,000,000) term loan facility and (ii) a
HK$195,000,000 (US$25,000,000) revolving loan facility, both with a
term of 18 months and an annual interest rate of 1.25% over HIBOR.
The second credit facility included (i) a HK$78,000,000
(US$10,000,000) term loan facility and (ii) a HK$117,000,000
(US$15,000,000) revolving loan facility, both with a term of 18
months and an annual interest rate of 1.25% over HIBOR. The term
loans from the first and second credit facilities were repaid in
May 2018. Both revolving loan facilities were terminated in August
2018.
(iii) 3-year revolving loan facility and 3-year term loan and revolving loan facilities
In November 2018, the Group through its subsidiary renewed a
3-year revolving loan facility with a bank in the aggregate amount
of HK$234,000,000 (US$30,000,000) with an annual interest rate of
0.85% over HIBOR. This credit facility is guaranteed by the
Company. As at June 30, 2019 and December 31, 2018, no amount has
been drawn from the revolving loan facility.
In May 2019, the Group through its subsidiary, entered into a
separate facility agreement with the bank for the provision of
additional unsecured credit facilities in the aggregate amount of
HK$400,000,000 (US$51,282,000). The 3-year credit facilities
include (i) a HK$210,000,000 (US$26,923,000) term loan facility and
(ii) a HK$190,000,000 (US$24,359,000) revolving loan facility, both
with an annual interest rate of 0.85% over HIBOR, and an upfront
fee of HK$819,000 (US$105,000) on the term loan. These credit
facilities are guaranteed by the Company. As at June 30, 2019, no
amount has been drawn from either of these credit facilities.
The Group's bank borrowings are repayable as from the dates
indicated as follows:
December
June 30, 31,
2019 2018
---------- ---------
(in US$'000)
Not later than 1 year - -
Between 1 to 2 years - 26,923
---------- ---------
- 26,923
================================== =========
As at June 30, 2019 and December 31, 2018, the Group had
unutilized bank borrowing facilities of HK$1,141,000,000
(US$146,282,000) and HK$931,000,000 (US$119,359,000)
respectively.
12. Commitments and Contingencies
Capital commitments
The Group had the following capital commitments:
June 30, 2019
--------------
(in US$'000)
Property, plant and equipment
Contracted but not provided for 3,679
==============
The Group does not have any other significant commitments or
contingencies.
13. Ordinary Shares
Pursuant to a resolution passed in the Annual General Meeting on
April 24, 2019, the Company's authorized share capital was
increased from US$75,000,000 to US$150,000,000 by the addition of
75,000,000 ordinary shares of US$1.00 each (equivalent to
750,000,000 ordinary shares of US$0.10 each after the share split
effective on May 30, 2019) in the share capital of the Company.
Pursuant to a resolution passed in the Extraordinary General
Meeting on May 29, 2019, with effect from May 30, 2019, each
ordinary share of the Company was subdivided into 10 ordinary
shares and the par value per ordinary share was changed from
US$1.00 to US$0.10. All Company ordinary share and per share
amounts presented were adjusted retroactively as the share split
was effective when the interim unaudited condensed consolidated
financial statements were issued.
As at June 30, 2019, the Company is authorized to issue
1,500,000,000 ordinary shares.
A summary of ordinary share transactions (in thousands) is as
follows:
2019 2018
-------- --------
As at January 1 666,577 664,470
Share option exercises - 856
-------- --------
As at June 30 666,577 665,326
======== ========
Each ordinary share is entitled to one vote. The holders of
ordinary shares are also entitled to receive dividends whenever
funds are legally available and when declared by the Board of
Directors of the Company.
14. Share-based Compensation
(i) Share-based Compensation of the Company
The Company conditionally adopted a share option scheme on June
4, 2005 (as amended on March 21, 2007) and such scheme has a term
of 10 years. It expired in 2016 and no further share options can be
granted. Another share option scheme was conditionally adopted on
April 24, 2015 (the "HCML Share Option Scheme"). Pursuant to the
HCML Share Option Scheme, the Board of Directors of the Company
may, at its discretion, offer any employees and directors
(including Executive and Non-executive Directors but excluding
Independent Non-executive Directors) of the Company, holding
companies of the Company and any of their subsidiaries or
affiliates, and subsidiaries or affiliates of the Company share
options to subscribe for shares of the Company.
As at June 30, 2019, the aggregate number of shares issuable
under the HCML Share Option Scheme is 23,130,970 ordinary shares
and the aggregate number of shares issuable under the prior share
option scheme which expired in 2016 is 1,845,180 ordinary shares.
Additionally, the number of shares authorized but unissued was
833,422,550 ordinary shares.
Share options granted are generally subject to a four-year
vesting schedule, depending on the nature and the purpose of the
grant. Share options subject to the four-year vesting schedule, in
general, vest 25% upon the first anniversary of the vesting
commencement date as defined in the grant letter, and 25% every
subsequent year. However, certain share option grants may have a
different vesting schedule as approved by the Board of Directors of
the Company. No outstanding share options will be exercisable or
subject to vesting after the expiry of a maximum of eight to ten
years from the date of grant.
A summary of the Company's share option activity and related
information is as follows:
Weighted average
Number of Weighted average remaining Aggregate
share exercise price in contractual life intrinsic value
options GBP per share (years) (in GBP'000)
------------ ------------------- ------------------ -----------------
Outstanding at January 1, 2018 11,264,120 1.77 6.29 43,158
Granted 10,606,260 4.69
Exercised (2,107,080) 1.40
Cancelled (1,208,450) 4.30
------------
Outstanding at December 31, 2018 18,554,850 3.31 7.35 15,158
============
Granted 180,000 4.22
Cancelled (648,090) 4.65
Expired (59,850) 4.65
------------
Outstanding at June 30, 2019 18,026,910 3.28 6.79 15,817
============
Vested and exercisable at December 31, 2018 8,032,040 1.68 4.84 14,843
Vested and exercisable at June 30, 2019 10,270,760 2.29 5.29 15,570
In estimating the fair value of share options granted, the
following assumptions were used in the Polynomial model for awards
granted in the periods indicated:
Year Ended December 31, Six Months Ended June 30,
--------------------------------------
2011 2013 2016 2017 2018 2019
------ ------ ------ ------ ------ --------------------------
Weighted average grant date fair value of share
options (in GBP per share) 0.18 0.32 0.90 1.27 1.67 1.51
Significant inputs into the valuation model
(weighted average):
Exercise price (in GBP per share) 0.44 0.61 1.97 3.11 4.69 4.22
Share price at effective date of grant (in GBP
per share) 0.43 0.61 1.97 3.11 4.66 4.22
Expected volatility (note (a)) 46.6% 36.0% 39.0% 36.3% 37.6% 37.7%
Risk-free interest rate (note (b)) 3.13% 3.16% 1.00% 1.17% 1.46% 1.08%
Contractual life of share options (in years) 10 10 8 10 10 10
Expected dividend yield (note (c)) 0% 0% 0% 0% 0% 0%
Notes:
(a) The Company calculated its expected volatility with
reference to the historical volatility prior to the issuances of
share options.
(b) The risk-free interest rates used in the Polynomial model
are with reference to the sovereign yield of the United Kingdom
because the Company's ordinary shares are currently listed on AIM
and denominated in GBP.
(c) The Company has not declared or paid any dividends and does
not currently expect to do so in the foreseeable future, and
therefore uses an expected dividend yield of zero in the Polynomial
model.
The Company will issue new shares to satisfy share option
exercises. The following table summarizes the Company's share
option exercises:
Six Months Ended
June 30,
--------------------
2019 2018
--------- ---------
(in US$'000)
Cash received from share options exercised - 720
Total intrinsic value of share options exercised - 4,817
The Group recognizes compensation expense on a graded vesting
approach over the requisite service period. The following table
presents share-based compensation expense included in the Group's
condensed consolidated statements of operations:
Six Months Ended
June 30,
-------------------
2019 2018
--------- --------
(in US$'000)
Research and development expenses 3,756 2,616
Administrative expenses 371 175
--------- --------
4,127 2,791
========= ========
As at June 30, 2019, the total unrecognized compensation cost
was US$10,391,000, and will be recognized on a graded vesting
approach over the weighted average remaining service period of 2.86
years.
(ii) LTIP
The Company grants awards under the LTIP to participating
directors and employees, giving them a conditional right to receive
ordinary shares of the Company or the equivalent ADS (collectively
the "Awarded Shares") to be purchased by the Trustee up to a cash
amount. Vesting will depend upon continued employment of the award
holder with the Group and will otherwise be at the discretion of
the Board of Directors of the Company. Additionally, some awards
are subject to change based on annual performance targets prior to
their determination date.
LTIP awards prior to the determination date
Performance targets vary by award, and may include targets for
shareholder returns, free cash flows, revenues, net profit after
taxes and the achievement of clinical and regulatory milestones. As
the extent of achievement of the performance targets is uncertain
prior to the determination date, a probability based on
management's assessment on the achievement of the performance
target has been assigned to calculate the amount to be recognized
as an expense over the requisite period with a corresponding entry
to liability.
LTIP awards after the determination date
Upon the determination date, the Company will pay a determined
monetary amount, up to the maximum cash amount based on the actual
achievement of the performance target specified in the award, to
the Trustee to purchase the Awarded Shares. Any cumulative
compensation expense previously recognized as a liability will be
transferred to additional paid-in capital, as an equity-settled
award. If the performance target is not achieved, no Awarded Shares
of the Company will be purchased and the amount previously recorded
in the liability will be reversed through share-based compensation
expense.
Granted awards under the LTIP are as follows:
Maximum cash
amount per annum Covered Performance target
Grant date (in US$ millions) financial years determination date
---------------------------------- ------------------- ----------------- --------------------
October 19, 2015 1.8 2014-2016 note (a)
March 24, 2016 0.3 note (b) note (b)
March 15, 2017 0.4 note (c) note (c)
March 15, 2017 and August 2, 2017 6.0 2017-2019 note (d)
December 15, 2017 0.5 2018-2019 note (d)
August 6, 2018 0.1 2018-2019 note (d)
December 14, 2018 1.5 2019 note (d)
Notes:
(a) The annual performance target determination date is the date
of the announcement of the Group's annual results for the covered
financial year and vesting occurs one business day after the
publication date of the annual report of the Company for the
financial year falling two years after the covered financial year
to which the LTIP award relates.
(b) This award does not stipulate performance targets and is
subject to a vesting schedule of 25% on each of the first, second,
third and fourth anniversaries of the date of grant.
(c) This award did not stipulate performance targets and vested
one business day after the publication date of the annual report
for the 2017 financial year.
(d) The annual performance target determination date is the date
of the announcement of the Group's annual results for the covered
financial year and vesting occurs two business days after the
announcement of the Group's annual results for the financial year
falling two years after the covered financial year to which the
LTIP award relates.
The Trustee has been set up solely for the purpose of purchasing
and holding the Awarded Shares during the vesting period on behalf
of the Group using funds provided by the Group. On the
determination date, if any, the Company will determine the cash
amount, based on the actual achievement of each annual performance
target, for the Trustee to purchase the Awarded Shares. The Awarded
Shares will then be held by the Trustee until they are vested.
The Trustee's assets include treasury shares and funds for
additional treasury shares, trustee fees and expenses. The number
of treasury shares (in the form of ordinary shares or ADS of the
Company) purchased and held by the Trustee were as follows:
Number of
treasury Cost
shares (in US$'000)
---------- --------------
As at January 1, 2018 559,775 1,957
Purchased 795,005 5,451
Vested (233,750) (731)
---------- --------------
As at December 31, 2018 1,121,030 6,677
Purchased 60,430 346
Vested (240,150) (944)
---------- --------------
As at June 30, 2019 941,310 6,079
========== ==============
For the six months ended June 30, 2019 and 2018, US$254,000 and
US$93,000 of the LTIP awards were forfeited respectively.
The following table presents the share-based compensation
expenses recognized under the LTIP awards:
Six Months Ended June 30,
----------------------------
2019 2018
------------- -------------
(in US$'000)
Research and development expenses 543 878
Selling and administrative expenses 827 723
------------- -------------
1,370 1,601
============= =============
Recorded with a corresponding credit
to:
Liability 590 789
Additional paid-in capital 780 812
------------- -------------
1,370 1,601
============= =============
For the six months ended June 30, 2019 and 2018, US$526,000 and
US$1,770,000 were reclassified from liability to additional paid-in
capital respectively upon LTIP awards reaching the determination
date. As at June 30, 2019 and December 31, 2018, US$1,299,000 and
US$1,235,000 were recorded as liabilities respectively for LTIP
awards prior to the determination date.
As at June 30, 2019, the total unrecognized compensation cost
was approximately US$3,624,000, which considers expected
performance targets and the amount expected to vest, and will be
recognized over the requisite periods.
15. Revenues
The following table presents disaggregated revenue:
Six Months Ended June 30, 2019
-----------------------------------
Innovation Commercial
Platform Platform Total
------------ ----------- --------
(in US$'000)
Goods-Manufacturing 2,994 - 2,994
Goods-Distribution - 87,596 87,596
Services 7,308 2,584 9,892
Royalties 1,715 - 1,715
------------ ----------- --------
12,017 90,180 102,197
============ =========== ========
Third parties 11,765 86,448 98,213
Related parties (Note 17(i)) 252 3,732 3,984
------------ ----------- --------
12,017 90,180 102,197
============ =========== ========
Six Months Ended June 30, 2018
-----------------------------------
Innovation Commercial
Platform Platform Total
------------ ----------- --------
(in US$'000)
Goods-Distribution - 82,912 82,912
Services 13,624 5,653 19,277
------------ ----------- --------
13,624 88,565 102,189
============ =========== ========
Third parties 8,548 85,116 93,664
Related parties (Note 17(i)) 5,076 3,449 8,525
------------ ----------- --------
13,624 88,565 102,189
============ =========== ========
16. Research and Development Expenses
Research and development expenses are summarized as follows:
Six Months Ended June
30,
------------------------
2019 2018
----------- -----------
(in US$'000)
Clinical trial related costs 43,707 40,244
Personnel compensation and related costs 21,917 17,282
Other research and development expenses 3,663 2,527
----------- -----------
69,287 60,053
=========== ===========
17. Significant Transactions with Related Parties and
Non-Controlling Shareholders of Subsidiaries
The Group has the following significant transactions with
related parties and non-controlling shareholders of subsidiaries,
which were carried out in the normal course of business at terms
determined and agreed by the relevant parties.
(i) Transactions with related parties:
Six Months Ended June
30,
------------------------
2019 2018
----------- -----------
(in US$'000)
Sales to:
Indirect subsidiaries of CK Hutchison 3,732 3,449
=========== ===========
Revenue from research and development services
from:
Equity investees 252 5,076
=========== ===========
Purchases from:
Equity investees 1,222 1,197
=========== ===========
Rendering of marketing services from:
Indirect subsidiaries of CK Hutchison 198 256
An equity investee 2,682 6,561
----------- -----------
2,880 6,817
=========== ===========
Rendering of support services from:
An indirect subsidiary of CK Hutchison 465 455
=========== ===========
(ii) Balances with related parties included in:
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Accounts receivable-related parties
Indirect subsidiaries of CK Hutchison (note
(a)) 1,794 2,709
An equity investee (note (a)) - 73
--------- ---------
1,794 2,782
========= =========
Accounts payable
An equity investee (note (a)) 2,796 6,507
========= =========
Amounts due from related parties
Equity investees (note (a)) 894 889
========= =========
Amounts due to related parties
An indirect subsidiary of CK Hutchison
(note (b)) 290 432
========= =========
Other deferred income
An equity investee (note (c)) 1,245 1,356
========= =========
Notes:
(a) Balances with related parties are unsecured, repayable on
demand and interest--free. The carrying values of balances with
related parties approximate their fair values due to their
short--term maturities.
(b) Amounts due to an indirect subsidiary of CK Hutchison are
unsecured, repayable on demand and interest-bearing if not settled
within one month.
(c) Other deferred income represents amounts recognized from
granting of promotion and marketing rights.
(iii) Transactions with non-controlling shareholders of subsidiaries:
Six Months Ended June
30,
------------------------
2019 2018
----------- -----------
(in US$'000)
Sales 12,146 10,506
=========== ===========
Purchases 6,397 8,113
=========== ===========
Interest expense - 39
=========== ===========
Dividend paid 1,282 -
=========== ===========
(iv) Balances with non-controlling shareholders of subsidiaries included in:
December
June 30, 31,
2019 2018
--------- ---------
(in US$'000)
Accounts receivable-third parties 5,631 5,070
========= =========
Accounts payable 4,132 4,960
========= =========
Other payables, accruals and advance receipts
Dividend payable - 1,282
========= =========
Other non-current liabilities
Loan 579 579
========= =========
18. Income Taxes
Six Months Ended June
30,
------------------------
2019 2018
----------- -----------
(in US$'000)
Current tax
HK (note (a)) 220 289
PRC (note (b)) 822 1,010
U.S. (note (c)) 347 104
Deferred income tax 1,073 1,277
----------- -----------
Income tax expense 2,462 2,680
=========== ===========
Notes:
(a) The Company, two subsidiaries incorporated in the British
Virgin Islands and its Hong Kong subsidiaries are subject to Hong
Kong profits tax which has been provided for at the rate of 16.5%
on the estimated assessable profits less estimated available tax
losses in each entity.
(b) Taxation in the PRC has been provided for at the applicable
rate on the estimated assessable profits less estimated available
tax losses, if any, in each entity. Under the PRC Enterprise Income
Tax Law (the "EIT Law"), the standard enterprise income tax rate is
25%. In addition, the EIT Law provides for, among others, a
preferential tax rate of 15% for companies which qualify as HNTE.
Hutchison MediPharma Limited and its wholly-owned subsidiary
Hutchison MediPharma (Suzhou) Limited qualify as a HNTE up to
December 31, 2019 and 2020 respectively.
Pursuant to the EIT law, a 10% withholding tax is levied on
dividends paid by PRC companies to their foreign investors. A lower
withholding tax rate of 5% is applicable under the China-HK Tax
Arrangement if direct foreign investors with at least 25% equity
interest in the PRC companies are Hong Kong tax residents, and meet
the conditions or requirements pursuant to the relevant PRC tax
regulations regarding beneficial ownership. Since the equity
holders of the major subsidiaries and equity investees of the
Company are Hong Kong incorporated companies and Hong Kong tax
residents, and meet the aforesaid conditions or requirements, the
Company has used 5% to provide for deferred tax liabilities on
retained earnings which are anticipated to be distributed. As at
June 30, 2019 and December 31, 2018, the amounts accrued in
deferred tax liabilities relating to withholding tax on dividends
were determined on the basis that 100% of the distributable
reserves of the major subsidiaries and equity investees operating
in the PRC will be distributed as dividends.
(c) The Company's subsidiary in the U.S. with operations in New
York State is subject to U.S. federal and state taxes, and have
been provided for at approximately 21% and 9% on the estimated
assessable profit respectively. Certain income receivable by the
Company is subject to U.S. withholding tax of 30%.
The reconciliation of the Group's reported income tax expense to
the theoretical tax amount that would arise using the tax rates of
the Company against the Group's loss before income taxes and equity
in earnings of equity investees is as follows:
Six Months Ended June
30,
------------------------
2019 2018
----------- -----------
(in US$'000)
Loss before income taxes and equity in earnings
of equity investees (68,301) (50,495)
=========== ===========
Tax calculated at the statutory tax rate
of the Company (11,270) (8,332)
Tax effects of:
Different tax rates available in different
jurisdictions 1,351 893
Tax valuation allowance 13,309 10,231
Preferential tax deduction (2,908) (1,763)
Expenses not deductible for tax purposes 1,094 690
Utilization of previously unrecognized tax
losses (49) (2)
Withholding tax on undistributed earnings
of PRC entities 1,386 1,323
Others (451) (360)
----------- -----------
Income tax expense 2,462 2,680
=========== ===========
19. Losses per Share
(i) Basic losses per share
Basic losses per share is calculated by dividing the net loss
attributable to the Company by the weighted average number of
outstanding ordinary shares in issue during the period. Treasury
shares held by the Trustee are excluded from the weighted average
number of outstanding ordinary shares in issue for purposes of
calculating basic losses per share.
Six Months Ended June
30,
--------------------------
2019 2018
------------ ------------
Weighted average number of outstanding
ordinary shares in issue 665,553,637 663,894,540
============ ============
Net loss attributable to the Company (US$'000) (45,369) (32,691)
------------ ------------
Losses per share attributable to the Company
(US$ per share) (0.07) (0.05)
------------ ------------
(ii) Diluted losses per share
Diluted losses per share is calculated by dividing net loss
attributable to the Company by the weighted average number of
outstanding ordinary shares in issue and dilutive ordinary share
equivalents outstanding during the period. Dilutive ordinary share
equivalents include shares issuable upon the exercise or settlement
of share option and LTIP awards issued by the Company using the
treasury stock method.
For the six months ended June 30, 2019 and 2018, the share
options and LTIP awards issued by the Company were not included in
the calculation of diluted losses per share because of their
anti-dilutive effect. Therefore, diluted losses per share was equal
to basic losses per share for the six months ended June 30, 2019
and 2018.
Note: The losses per share attributable to the Company-basic and
diluted presented were adjusted retroactively for each of the six
months ended June 30, 2019 and 2018 to take into account the share
split approved by ordinary resolution at the Extraordinary General
Meeting of the Company held on May 29, 2019, pursuant to which each
ordinary share was subdivided into 10 ordinary shares with effect
from May 30, 2019.
20. Segment Reporting
The Group determines its operating segments from both business
and geographic perspectives as follows:
(i) Innovation Platform (Drug R&D): focuses on discovering,
developing and commercializing targeted therapeutics in oncology
and autoimmune diseases, and the provision of research and
development services; and
(ii) Commercial Platform: comprises of the manufacture,
marketing and distribution of prescription and over-the-counter
pharmaceuticals in the PRC as well as consumer health products
through Hong Kong. The Commercial Platform is further segregated
into two core business areas:
(a) Prescription Drugs: comprises the development, manufacture,
distribution, marketing and sale of prescription pharmaceuticals;
and
(b) Consumer Health: comprises the development, manufacture,
distribution, marketing and sale of over-the-counter
pharmaceuticals and consumer health products.
Innovation Platform and Prescription Drugs businesses under the
Commercial Platform are primarily located in the PRC. The locations
for Consumer Health business under the Commercial Platform are
further segregated into the PRC and Hong Kong.
The performance of the reportable segments is assessed based on
three measurements: (a) losses or earnings of subsidiaries before
interest income, interest expense, income tax expenses and equity
in earnings of equity investees, net of tax ("Adjusted (LBIT)/EBIT"
or "Adjusted LBIT"), (b) equity in earnings of equity investees,
net of tax and (c) operating (loss)/profit.
The segment information is as follows:
Six Months Ended June 30, 2019
------------------------------------------------------------------------------------
Innovation
Platform Commercial Platform
----------- --------------------------------------------
Prescription
Drug R&D Drugs Consumer Health
----------- ------------- ------------------
PRC PRC PRC Hong Kong Subtotal Unallocated Total
----------- ------------- ------ ---------- --------- ------------ -----------
(in US$'000)
Revenue from external
customers 12,017 72,618 6,192 11,370 90,180 - 102,197
----------- ------------- ------ ---------- --------- ------------ -----------
Adjusted (LBIT)/EBIT (64,231) 2,191 464 971 3,626 (10,069) (70,674)
Interest income 205 30 16 2 48 2,808 3,061
Equity in earnings
of equity investees,
net of tax 176 21,027 6,105 - 27,132 - 27,308
----------- ------------- ------ ---------- --------- ------------ -----------
Operating (loss)/profit (63,850) 23,248 6,585 973 30,806 (7,261) (40,305)
Interest expense - - - - - 688 688
Income tax expense 120 624 138 142 904 1,438 2,462
Net (loss)/income
attributable to
the Company (63,813) 21,815 5,542 385 27,742 (9,298) (45,369)
Depreciation/amortization 2,191 80 11 45 136 78 2,405
Additions to non-current
assets (other than
financial instruments
and deferred tax
assets) 3,300 2,624 9 3 2,636 7 5,943
=========== ============= ====== ========== ========= ============ ===========
As at June 30, 2019
-------------------------------------------------------------------------------------
Innovation
Platform Commercial Platform
----------- ---------------------------------------------------
Prescription
Drug R&D Drugs Consumer Health
----------- ------------- -------------------
PRC PRC PRC Hong Kong Subtotal Unallocated Total
----------- ------------- ------- ---------- --------- -------------- ---------
(in US$'000)
Total assets 97,488 134,002 65,790 11,626 211,418 186,308 495,214
Property, plant
and equipment 16,317 347 69 345 761 591 17,669
Right-of-use assets 2,753 2,381 34 463 2,878 1,161 6,792
Leasehold land 1,157 - - - - - 1,157
Goodwill - 2,779 407 - 3,186 - 3,186
Other intangible
asset - 315 - - 315 - 315
Investments in
equity investees 8,689 78,593 59,695 - 138,288 - 146,977
=========== ============= ======= ========== ========= ============== =========
Six Months Ended June 30, 2018
---------------------------------------------------------------------------------------
Innovation
Platform Commercial Platform
------------- ---------------------------------------------
Prescription
Drug R&D Drugs Consumer Health
------------- -------------- ------------------
PRC PRC PRC Hong Kong Subtotal Unallocated Total
------------- -------------- ------ ---------- --------- ------------ -----------
(in US$'000)
Revenue from external
customers 13,624 67,950 6,559 14,056 88,565 - 102,189
------------- -------------- ------ ---------- --------- ------------ -----------
Adjusted (LBIT)/EBIT (50,718) 3,457 456 1,584 5,497 (7,619) (52,840)
Interest income 26 23 7 32 62 2,701 2,789
Equity in earnings of
equity investees, net of
tax (2,349) 19,408 5,991 - 25,399 - 23,050
------------- -------------- ------ ---------- --------- ------------ -----------
Operating (loss)/profit (53,041) 22,888 6,454 1,616 30,958 (4,918) (27,001)
Interest expense - - - 39 39 405 444
Income tax expense 20 813 124 264 1,201 1,459 2,680
Net (loss)/income
attributable to the
Company (52,930) 20,768 5,497 649 26,914 (6,675) (32,691)
Depreciation/amortization 1,584 68 12 10 90 14 1,688
Additions to non-current
assets (other than
financial instruments and
deferred tax assets) 1,564 5 7 14 26 5 1,595
============= ============== ====== ========== ========= ============ ===========
As at December 31, 2018
-----------------------------------------------------------------------------------------------
Innovation
Platform Commercial Platform
------------------ ---------------------------------------------------
Drug R&D Prescription Drugs Consumer Health
------------------ ------------------- -------------------
PRC PRC PRC Hong Kong Subtotal Unallocated Total
------------------ ------------------- ------- ---------- --------- ------------ --------
(in US$'000)
Total assets 100,388 118,445 67,352 11,686 197,483 234,247 532,118
Property, plant
and equipment 15,223 204 71 418 693 700 16,616
Leasehold land 1,174 - - - - - 1,174
Goodwill - 2,779 407 - 3,186 - 3,186
Other intangible
asset - 347 - - 347 - 347
Investments in
equity investees 8,514 68,812 60,992 - 129,804 - 138,318
================== =================== ======= ========== ========= ============ ========
Revenue from external customers is after elimination of
inter--segment sales. Sales between segments are carried out at
mutually agreed terms.
There was one customer which accounted for over 10% of the
Group's revenue for the six months ended June 30, 2019 and 2018
respectively.
Unallocated expenses mainly represent corporate expenses which
include corporate employee benefit expenses and the relevant
share-based compensation expenses. Unallocated assets mainly
comprise cash and cash equivalents and short-term investments.
A reconciliation of Adjusted LBIT to net loss is as follows:
Six Months Ended
June 30,
--------------------
2019 2018
--------- ---------
(in US$'000)
Adjusted LBIT (70,674) (52,840)
Interest income 3,061 2,789
Equity in earnings of equity investees, net
of tax 27,308 23,050
Interest expense (688) (444)
Income tax expense (2,462) (2,680)
--------- ---------
Net loss (43,455) (30,125)
========= =========
21. Note to Condensed Consolidated Statements of Cash Flows
Reconciliation of net loss for the period to net cash used in
operating activities:
Six Months Ended
June 30,
--------------------
2019 2018
--------- ---------
(in US$'000)
Net loss (43,455) (30,125)
Adjustments to reconcile net loss to net
cash used in operating activities
Depreciation and amortization 2,405 1,688
Share-based compensation expense-share options 4,127 2,791
Share-based compensation expense-LTIP 1,370 1,601
Equity in earnings of equity investees, net
of tax (27,308) (23,050)
Dividends received from equity investees 18,173 23,526
Changes in right-of-use assets (929) -
Other adjustments 1,107 990
Changes in working capital
Accounts receivable-third parties (2,562) (6,053)
Inventories (2,113) 2,041
Accounts payable 520 (5,057)
Other payables, accruals and advance receipts 14,606 10,215
Lease liabilities 764 -
Other changes in working capital 3,250 2,837
--------- ---------
Total changes in working capital 14,465 3,983
--------- ---------
Net cash used in operating activities (30,045) (18,596)
========= =========
22. Litigation
From time to time, the Group may become involved in litigation
relating to claims arising from the ordinary course of business.
The Group believes that there are currently no claims or actions
pending against the Group, the ultimate disposition of which could
have a material adverse effect on the Group's results of
operations, financial position or cash flows. However, litigation
is subject to inherent uncertainties and the Group's view of these
matters may change in the future. When an unfavorable outcome
occurs, there exists the possibility of a material adverse impact
on the Group's financial position and results of operations for the
periods in which the unfavorable outcome occurs, and potentially in
future periods.
On May 17, 2019, Luye Pharma Hong Kong Ltd. issued a notice to
the Group purporting to terminate a distribution agreement that
granted the Group exclusive commercial rights to Seroquel in the
PRC for failure to meet a pre-specified target. The Group disagrees
with this assertion and believes that they have no basis for
termination, and therefore intends to enforce its rights under the
current agreement. On July 29, 2019, the Group initiated
arbitration in Hong Kong. Accordingly, no adjustment has been made
to Seroquel-related balances as at June 30, 2019, including
accounts receivable, inventories, long-term prepayment and accounts
payable of US$1.1 million, US$0.1 million, US$1.2 million and
US$2.2 million respectively.
23. Subsequent Events
The Group evaluated subsequent events through July 30, 2019,
which is the date when the interim unaudited condensed consolidated
financial statements were issued.
This information is provided by RNS, the news service of the
London Stock Exchange. RNS is approved by the Financial Conduct
Authority to act as a Primary Information Provider in the United
Kingdom. Terms and conditions relating to the use and distribution
of this information may apply. For further information, please
contact rns@lseg.com or visit www.rns.com.
END
IR EALXEDSLNEEF
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