Krystal Biotech, Inc. (the “Company”) (NASDAQ: KRYS), a
commercial-stage biotechnology company, announced today clinical
data updates for both KB408 and KB407, the Company’s
clinical-stage, inhaled genetic medicine programs in Phase 1 for
the treatment of rare respiratory diseases. Today’s updates include
molecular data from multiple patients demonstrating SERPINA1
delivery and alpha-1 antitrypsin (AAT) expression within the
respiratory tract following KB408 administration as well as safety
and tolerability data for both KB407 and KB408 that, taken
together, highlight the potential of the Company’s platform to
safely deliver genetic cargo to the lung.
“To achieve meaningful AAT expression levels and functionality
with the first dose of KB408 is a very exciting development for
this program and for our alpha-1 antitrypsin deficiency (AATD)
patients,” said Robert A. Sandhaus, MD, PhD, FCCP, Professor of
Medicine at the National Jewish Health in Denver, Executive Vice
President and Senior Medical Director of AlphaNet, as well as
Clinical Director of the Alpha-1 Foundation. “Even though the first
intravenous augmentation therapy was approved decades ago, we still
don’t have a good understanding of the impact these therapies are
having on lung disease. A safe, effective, non-invasive therapy
that is less burdensome on patients and supported by molecular
evidence of function in the lung is needed, and we look forward to
additional clinical updates on KB408 in the months to come.”
The Company will host an investor conference call and webcast
today, Thursday, December 12, 2024, at 8:30 am ET, to discuss the
clinical data updates. Investors and the general public can access
the live webcast at:
https://www.webcaster4.com/Webcast/Page/3018/51767. For those
unable to listen to the live webcast, an archived version will also
be available on the Investors section of the Company’s website for
at least 30 days.
KB408 for the treatment of alpha-1 antitrypsin
deficiency (AATD) lung disease
KB408 is being evaluated in the Company’s Phase 1 SERPENTINE-1
study. SERPENTINE-1 is an open label, single dose escalation study
in adult patients with AATD with a Pi*ZZ or a Pi*ZNull genotype.
SERPENTINE-1 is designed to include up to three dose escalation
cohorts evaluating single administrations of 109, 1010, and 1011
PFU of KB408 via inhalation. Additional details of the
SERPENTINE-1 study can be found
at www.clinicaltrials.gov under NCT identifier
NCT06049082.
As of the December 6, 2024 data cut-off, a total of seven (7)
patients had been enrolled in SERPENTINE-1, including 3 patients in
Cohort 1 who had received the 109 PFU KB408 dose and 4 patients in
Cohort 2 who had received the 1010 PFU KB408 dose. One patient in
each of Cohort 1 and Cohort 2 were receiving background intravenous
(IV) augmentation therapy.
Two patients in Cohort 2 also received bronchoscopies to assess
SERPINA1 delivery and AAT levels in the lung. Both a baseline
bronchoscopy and a post-dose bronchoscopy, conducted 24 to 48 hours
after KB408 dosing, were completed. One of the two patients who
received bronchoscopies was receiving background IV augmentation
therapy.
Clear evidence of successful gene delivery was observed in both
patients, including high rates of transduction and AAT expression
in the conducting airways of both patients as assessed via
bronchoscopy. Key molecular findings for each patient are
summarized below:
Patient Not on Background IV Augmentation
- A clinically meaningful proportion of conducting airway
epithelial cells were transduced following administration of a
single dose of KB408, with the percentage of cells positive for AAT
expression increasing from 0% at baseline to 39% after KB408
dosing.
- Free AAT levels in lung epithelial lining fluid increased over
8-fold, rising from 85 nM at baseline to 729 nM after KB408
dosing.
- AAT functionality was also confirmed by detection of AAT-NE
binding, with the percentage of active, unbound neutrophil elastase
in epithelial lining fluid dropping from 97.2% at baseline to 40.2%
– an over 50% absolute reduction achieved within 48 hours after
dosing.
Patient on Background IV Augmentation
- Again, a clinically meaningful proportion of conducting airway
epithelial cells were transduced following administration of a
single dose of KB408, with the percentage of cells positive for AAT
expression increasing from 3% at baseline to 35% after KB408
dosing.
- Lavage samples could not be successfully collected from this
patient, preventing accurate quantification of AAT and neutrophil
elastase binding in lung epithelial lining fluid. However, both
KB408 genomes and SERPINA1 RNA transcripts were detected in
multiple bronchial brushing samples, with an average of 4 x 103
genome copies and 4 x 102 transcript copies detected, providing
further support of successful gene delivery and expression in the
KB408 treated lung.
In addition to evidence of KB408 transduction and AAT expression
in the lungs of these two patients, increases in serum AAT levels
were also detected in all four Cohort 2 patients after KB408
dosing, suggestive of broad dissemination of KB408-encoded AAT
following expression in the lung. Increases in serum AAT relative
to baseline ranged from 270 nM to 5.3 µM in the three patients that
were not on confounding background IV augmentation, including in
one case increases in serum AAT from 4.4 µM at baseline to 9.7 µM
after KB408 dosing.
KB408-related adverse events for all seven patients treated in
Cohort 1 and Cohort 2 were mild to moderate and transient. No
serious adverse events have been reported.
“With clear evidence of gene delivery, including detection of
high nanomolar concentrations of AAT in lung epithelial lining
fluid, as well as corresponding reductions in the percentage of
unbound, active neutrophil elastase by over 50%, today’s initial
clinical data is a major step forward towards our goal of
developing a safe, effective, and non-invasive therapy for AATD
patients to maintain therapeutic AAT levels in the lung,” said Suma
Krishnan, President, Research & Development, Krystal Biotech,
Inc. “These data, together with the attractive tolerability profile
observed to date, also reinforce our conviction in HSV-1 based gene
delivery to the lung and our entire inhaled genetic medicines
pipeline. We look forward to sharing additional updates on our
respiratory programs in 2025.”
The Company will enroll two additional patients in Cohort 2 of
SERPENTINE-1 and expects to provide additional data updates in
2025. In parallel, the Company will open Cohort 3 to explore safety
and gene delivery at the highest dose of KB408.
KB407 for the treatment of cystic fibrosis
(CF)
Based on preclinical data submitted to date by the Company, the
Cystic Fibrosis Foundation (CFF) Therapeutic Development Network
(TDN) Clinical Research Executive Committee has granted conditional
sanctioning of the Company’s KB407 Phase 1 CORAL-1 study protocol
subject to review of the data monitoring committee charter, if
required, to align with CFF TDN standards. No additional
preclinical updates for KB407 are required, and the Company expects
to be fully sanctioned and open sites within the CFF TDN
shortly.
KB407 is being evaluated in the Phase 1 CORAL-1 study. CORAL-1
is an open label, dose escalation study in adult patients with CF.
CORAL-1 is designed to include up to three dose escalation cohorts
evaluating either one, two, or four daily administrations of 109
PFU of KB407 via inhalation. Additional details of the CORAL-1
study can be found at www.clinicaltrials.gov under NCT
identifier NCT05504837.
As of the December 6, 2024 data cut-off, a total of five (5)
patients had been enrolled in CORAL-1. Three patients received a
single 109 PFU KB407 dose in Cohort 1 and three patients, including
one roll-over from Cohort 1, received two daily 109 PFU KB407 doses
in Cohort 2. All but one patient was on background modulator
therapy.
The initial focus of Cohorts 1 and 2 was safety of single and
repeat inhaled administration of KB407 in patients with CF. As
observed with KB408, KB407 has been well tolerated in all patients
dosed to date. KB407-related adverse events for all five patients
treated in Cohort 1 and Cohort 2 were mild to moderate and
transient. No serious adverse events have been reported. The
Company expects to report data from Cohort 3 in 1H 2025, including
data on CFTR gene delivery and expression in patients with cystic
fibrosis.
About Krystal Biotech, Inc.
Krystal Biotech, Inc. (NASDAQ: KRYS) is a commercial-stage
biotechnology company focused on the discovery, development and
commercialization of genetic medicines to treat diseases with high
unmet medical needs. VYJUVEK® is the Company’s first commercial
product, the first-ever redosable gene therapy, and the first
medicine approved by the FDA for the treatment of dystrophic
epidermolysis bullosa. The Company is rapidly advancing a robust
preclinical and clinical pipeline of investigational genetic
medicines in respiratory, oncology, dermatology, ophthalmology, and
aesthetics. Krystal Biotech is headquartered in Pittsburgh,
Pennsylvania. For more information, please visit
http://www.krystalbio.com, and follow @KrystalBiotech on LinkedIn
and X (formerly Twitter).
Forward-Looking Statements
Any statements in this press release about future expectations,
plans and prospects for Krystal Biotech, Inc., including statements
about the potential of the Company’s platform to safely deliver
genetic cargo to the lung; the Company’s clinical-stage, inhaled
genetic medicines programs in Phase 1 for the treatment of rare
respiratory diseases; the Company’s plans to enroll two additional
patients in Cohort 2 of its SERPENTINE-1 study and provide
additional data updates in 2025; the Company’s plans to open Cohort
3 of its SERPENTINE-1 study to explore safety and gene delivery at
the highest dose of KB408; the Company’s expectation to be fully
sanctioned and open sites within the CFF TDN shortly; the Company’s
expectation that it will report data from Cohort 3 of its CORAL-1
study in 1H 2025, including data on CFTR gene delivery and
expression in cystic fibrosis patients; and other statements
containing the words “anticipate,” “believe,” “estimate,” “expect,”
“intend,” “may,” “plan,” “predict,” “project,” “target,”
“potential,” “likely,” “will,” “would,” “could,” “should,”
“continue,” and similar expressions, constitute forward-looking
statements within the meaning of The Private Securities Litigation
Reform Act of 1995. Actual results may differ materially from those
indicated by such forward-looking statements as a result of various
important factors, including uncertainties inherent in the
initiation and conduct of clinical trials, as well as regulatory
review of clinical trials and applications for marketing approvals;
and such other important factors as are set forth under the caption
“Risk Factors” in the Company’s annual and quarterly reports on
file with the U.S. Securities and Exchange Commission. The
forward-looking statements included in this press release represent
the Company’s views as of the date of this press release. The
Company anticipates that subsequent events and developments will
cause its views to change. However, while the Company may elect to
update these forward-looking statements at some point in the
future, it specifically disclaims any obligation to do so. These
forward-looking statements should not be relied upon as
representing the Company’s views as of any date subsequent to the
date of this press release.
CONTACTInvestors and
Media:Stéphane Paquette, PhDKrystal
Biotechspaquette@krystalbio.com
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