Windtree Announces Positive Phase 2b Topline Clinical Results with Istaroxime Significantly Improving Cardiac Function and Blood Pressure in Heart Failure Patients in Early Cardiogenic Shock
30 September 2024 - 10:15PM
Windtree Therapeutics, Inc. (“Windtree” or the “Company”)
(NasdaqCM: WINT), a biotechnology company focused on advancing
early and late-stage innovative therapies for critical conditions
and diseases, today announced positive topline clinical results for
its Phase 2b SEISMiC Extension Study of istaroxime in heart failure
patients in early cardiogenic shock.
Early cardiogenic shock is caused by a failing heart and is
characterized by low blood pressure, leaving the patient at risk of
developing inadequate blood flow to vital organs leading to high
morbidity and mortality. Istaroxime is a novel first-in-class
investigational therapy that is intended to improve systolic
contraction and diastolic relaxation of the heart while also
increasing blood pressure and maintaining renal function with a
generally favorable safety profile. Istaroxime has been studied in
four positive Phase 2 trials enrolling patients with acute heart
failure and early cardiogenic shock due to heart failure.
The Phase 2b SEISMiC Part B Extension Study in early cardiogenic
shock (SCAI Stage B) randomized 30 subjects and was conducted in
the United States, Europe and Latin America (3 subjects have been
discharged but have not completed their 30-day visit). The study is
focused on istaroxime’s observed ability to correct low blood
pressure and to improve cardiac function and other parameters over
96 hours of close monitoring with the final visit at 30 days. The
results build upon the positive results reported previously in the
Phase 2b SEISMiC Part A study. The Part B study included
hospitalized patients with SCAI Stage B cardiogenic shock with
persistent hypotension due to acute heart failure and evaluated two
different dose regimens of istaroxime compared to placebo. Patients
in the active treatment groups received infusions of istaroxime for
up to 60 hours, with one group receiving a decreasing istaroxime
dose over time and the second group receiving a constant istaroxime
dose. The study tested an extended dosing duration of istaroxime
compared to previous studies, where treatment was limited to 24
hours, to determine the potential for additional benefit and, along
with dose titration, to determine the optimal dosing regimen for an
anticipated late-stage Phase 3 clinical trial. For the primary
endpoint evaluating blood pressure, subjects from Part A and Part B
of SEISMiC were prospectively combined for analysis. In the
analysis of Part B, all istaroxime-treated patients were compared
to the placebo group. For certain endpoints in Part B, the
dose-response between the two different istaroxime dose regimens
was compared.
Topline study results:
- The study met its primary endpoint in significantly improving
systolic blood pressure over six hours (SBP AUC), with the combined
Part A and Part B SEISMiC istaroxime group performing significantly
better compared to the placebo group (62.0±7 vs 36.4±7 mmHg*hr, p =
0.0070). Despite the smaller number of patients in SEISMiC Part B,
the SBP AUC was also significantly improved by istaroxime compared
to placebo (78.4±12 vs. 39.6±14 mmHg*hr, p=0.0429).
- The improvements in SBP AUC at 24 hours in the combined Part A
and Part B analysis were also significantly increased by istaroxime
(292.4±24 vs 190.9±26 mmHg*hr, p=0.0031). In Part B alone, the
istaroxime group was significantly better compared to the placebo
group (299.3±48 vs 139.0±56mmHg*hr, (p = 0.0377). With the longer
istaroxime dosing in Part B, the SBP AUC was significantly improved
at 48 hours (594.4±95 vs 271.7±110, p = 0.0352) and 60 hours
(711.4±119 vs 320.4±138 mmHg*hr, p = 0.0408) as well.
SEISMiC Part B results:
- Cardiac output (the amount of blood pumped by the heart per
minute) was improved during the infusion by approximately 15% in
the istaroxime group over the course of treatment. Heart rate
tended to decrease and there was no statistically significant
increase in heart rate versus placebo in the istaroxime group. At
12 and 24 hours, patients in the istaroxime group experienced
statistically significant reductions in heart rate (p = 0.0102 and
p = 0.0218, respectively). Increasing heart rate contributes to
greater cardiac oxygen demand and workload, and therefore can lead
to deleterious effects in heart failure patients.
- Pulmonary capillary wedge pressure (PCWP) is elevated in this
patient population and also was elevated in our study subjects at
baseline. Istaroxime treatment reduced PCWP significantly more than
placebo within six hours (-6.6 vs -0.9 mmHg, p = 0.0001) and the
effect persisted through 60 hours. PCWP is a measure of cardiac
filling pressure and when high contributes to worsening heart
failure and pulmonary edema.
- Mixed venous oxygen saturation (SVO2), an assessment of organ
perfusion, was significantly improved by 12 hours (mean difference
of the istaroxime group compared to placebo was approximately 9%,
p=0.0071), and remained significant through 48 hours
(p=0.0001). The improvement versus placebo generally persisted
through a 60-hour assessment. A low SVO2 can indicate that cardiac
output is not high enough to meet the tissue oxygen needs.
- Renal function measured by estimated glomerular filtration rate
(eGFR) was improved in this study in the istaroxime group compared
to placebo at all time points reaching statistical significance at
48 hours (p =0.0291).
- Clinical signs and symptoms of congestion and heart failure
improved in both groups. The New York Heart Association (NYHA)
classification of heart failure severity significantly decreased in
the istaroxime group at 24 hours (p=0.020), 48 hours (p=0.035), and
72 hours (p=0.010) and was similar to placebo at 96 hours.
- Worsening heart failure reported as a serious adverse event
occurred less frequently in the istaroxime group compared to
placebo 5.3% versus 18.2%, respectively.
The istaroxime safety profile in Part B was favorable and
generally consistent with what has been previously reported in
other istaroxime clinical trials. Treatment-emergent adverse events
were reported more frequently in the istaroxime group at 78.9%
compared to 45.5% in the placebo group, predominantly due to
nausea, vomiting, infusion site discomfort and headache that have
been observed previously with istaroxime. Serious adverse events
were infrequent and occurred at a similar frequency in both the
istaroxime and placebo groups (10.5% vs. 27.3%, respectively).
Importantly, consistent with previous findings, istaroxime did not
increase clinically significant arrythmias compared to the placebo
group.
Alexandre Mebazaa. MD, PhD, FESC (Université Paris Cité,
France), Professor of Critical Care and heart failure expert,
said, “Innovation with drug therapy is needed in cardiogenic shock
treatment. Istaroxime has a unique profile. It may be the only drug
candidate that has been shown to simultaneously improve blood
pressure, cardiac output and renal function without increasing
heart rate or risk for cardiac arrhythmias. These are all desirable
attributes for a drug treating cardiogenic shock and acute heart
failure.”
Dr. Mebazaa will be joining the Company for a Virtual
Investor Day presentation of the above and other results,
a review of the program and the forward-looking strategy, plans and
milestones on Tuesday, October 1 at 3pm ET.
Register for the event here:
https://lifescievents.com/event/windtreetx/. The presentation will
be made available on Windtree’s website after the meeting.
“We are very pleased with the results of this SEISMiC
cardiogenic shock study. Through four positive Phase 2 studies in
acute heart failure, with and without early cardiogenic shock, in
over 300 patients treated with istaroxime to date, we have observed
a unique and attractive profile,” said Craig Fraser, CEO and
Chairman of Windtree Therapeutics. “We are excited to pursue the
next steps of development to potentially deliver an important
therapy for patients that need better treatments for this critical
condition.”
About IstaroximeIstaroxime is a first-in-class
dual-mechanism therapy designed to improve both systolic and
diastolic cardiac function. Istaroxime is designed as a positive
inotropic agent that increases myocardial contractility through
inhibition of Na+/K+- ATPase with a complimentary mechanism that
facilitates myocardial relaxation through activation of the SERCA2a
calcium pump on the sarcoplasmic reticulum enhancing calcium
reuptake from the cytoplasm. Data from multiple Phase 2 studies in
patients with early cardiogenic shock or acute decompensated heart
failure have demonstrated that istaroxime infused intravenously
significantly improves cardiac function and blood pressure without
increasing heart rate or the incidence of cardiac rhythm
disturbances.
About Windtree Therapeutics, Inc.Windtree
Therapeutics, Inc. is a biotechnology company focused on advancing
early and late-stage innovative therapies for critical conditions
and diseases. Windtree’s portfolio of product candidates includes
istaroxime, a Phase 2 candidate with SERCA2a activating properties
for acute heart failure and associated cardiogenic shock,
preclinical SERCA2a activators for heart failure and preclinical
precision aPKCi inhibitors that are being developed for potential
in rare and broad oncology applications. Windtree also has a
licensing business model with partnership out-licenses currently in
place.
Forward Looking StatementsThis press release
contains statements related to the potential clinical effects of
istaroxime; the potential benefits and safety of istaroxime; the
clinical development of istaroxime; and our research and
development program for treating patients in early cardiogenic
shock due to heart failure. Such statements constitute
forward-looking statements within the meaning of The Private
Securities Litigation Reform Act of 1995. The Company may, in some
cases, use terms such as “predicts,” “believes,” “potential,”
“proposed,” “continue,” “estimates,” “anticipates,” “expects,”
“plans,” “intends,” “may,” “could,” “might,” “will,” “should” or
other words that convey uncertainty of future events or outcomes to
identify these forward-looking statements. Such statements are
based on information available to the Company as of the date of
this press release and are subject to numerous important factors,
risks and uncertainties that may cause actual events or results to
differ materially from the Company’s current expectations. Examples
of such risks and uncertainties include, among other things: the
Company’s ability to secure significant additional capital as and
when needed; the Company’s ability to achieve the intended benefits
of the aPKCi asset acquisition with Varian Biopharmaceuticals,
Inc.; the Company’s risks and uncertainties associated with the
success and advancement of the clinical development programs for
istaroxime and the Company’s other product candidates, including
preclinical oncology candidates; the Company’s ability to access
the debt or equity markets; the Company’s ability to manage costs
and execute on its operational and budget plans; the results, cost
and timing of the Company’s clinical development programs,
including any delays to such clinical trials relating to enrollment
or site initiation; risks related to technology transfers to
contract manufacturers and manufacturing development activities;
delays encountered by the Company, contract manufacturers or
suppliers in manufacturing drug products, drug substances, and
other materials on a timely basis and in sufficient amounts; risks
relating to rigorous regulatory requirements, including that: (i)
the U.S. Food and Drug Administration or other regulatory
authorities may not agree with the Company on matters raised during
regulatory reviews, may require significant additional activities,
or may not accept or may withhold or delay consideration of
applications, or may not approve or may limit approval of the
Company’s product candidates, and (ii) changes in the national or
international political and regulatory environment may make it more
difficult to gain regulatory approvals and risks related to the
Company’s efforts to maintain and protect the patents and licenses
related to its product candidates; risks that the Company may never
realize the value of its intangible assets and have to incur future
impairment charges; risks related to the size and growth potential
of the markets for the Company’s product candidates, and the
Company’s ability to service those markets; the Company’s ability
to develop sales and marketing capabilities, whether alone or with
potential future collaborators; the rate and degree of market
acceptance of the Company’s product candidates, if approved; the
economic and social consequences of the COVID-19 pandemic and the
impacts of political unrest, including as a result of geopolitical
tension, including the conflict between Russia and Ukraine, the
People’s Republic of China and the Republic of China (Taiwan), and
the evolving events in Israel and Gaza, and any sanctions, export
controls or other restrictive actions that may be imposed by the
United States and/or other countries which could have an adverse
impact on the Company’s operations, including through disruption in
supply chain or access to potential international clinical trial
sites, and through disruption, instability and volatility in the
global markets, which could have an adverse impact on the Company’s
ability to access the capital markets. These and other risks are
described in the Company’s periodic reports, including its Annual
Report on Form 10-K, Quarterly Reports on Form 10-Q and Current
Reports on Form 8-K, filed with or furnished to the Securities and
Exchange Commission and available at www.sec.gov. Any
forward-looking statements that the Company makes in this press
release speak only as of the date of this press release. The
Company assumes no obligation to update forward-looking statements
whether as a result of new information, future events or otherwise,
after the date of this press release.
Contact Information:Eric
Curtisecurtis@windtreetx.com
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