Pharvaris (Nasdaq: PHVS), a late-stage biopharmaceutical company
developing novel, oral bradykinin B2 receptor antagonists to
prevent and treat hereditary angioedema (HAE) attacks, is
highlighting the differentiated profile of deucrictibant as a
prophylactic and on-demand treatment of HAE attacks at the
Bradykinin Symposium 2024, being held in Berlin from September 5-6,
2024. A summary of the data being presented at the congress can be
found here.
“Based on a snapshot analysis, treatment with deucrictibant led
to a 93% reduction in attack rate compared to study baseline, a
median attack rate of zero for every month, and a mean proportion
of attack-free days of 99% after more than a year of mean duration
of treatment in a prophylactic extension study. Together with the
improvements in disease control and health-related quality of life
observed in the randomized, placebo-controlled part of the
CHAPTER-1 study, these data underscore the potential of
deucrictibant to be an effective and well-tolerated prophylactic
agent in the treatment of HAE,” said Peng Lu, M.D., Ph.D., Chief
Medical Officer of Pharvaris. “Long-term extension data of
deucrictibant in the on-demand setting similarly confirm its
potential to become a preferred option for the treatment of HAE
attacks with a median onset of symptom relief of 1.1 hours, as
measured by Patient Global Impression of Change (PGI-C) and median
complete resolution of 11.5 hours, as measured by Patient Global
Impression of Severity (PGI-S). The rapid onset of symptom relief
reported in RAPIDe-2 and the results of a propensity score-matched
analysis favoring deucrictibant over standard of care provide
confidence in our ability to differentiate deucrictibant in the
on-demand HAE space. Lastly, the safety and tolerability profile of
deucrictibant has been reaffirmed in multiple nonclinical and
clinical studies.”
Marc A. Riedl, M.D., M.S., Professor of Medicine, Clinical
Director of the U.S. Hereditary Angioedema Association (HAEA)
Angioedema Center at the University of California San Diego (UCSD),
Clinical Service Chief for Allergy/Immunology at UCSD, added, “The
goal of HAE management is for affected individuals to live a normal
life, ensuring they can engage in all work, school, family, and
leisure activities as desired without limitation from angioedema
symptoms. Therapies that offer improved efficacy, tolerability, and
convenience have the potential to normalize the lives of people
living with HAE. These long-term extension and health-related
quality of life data, together with the Phase 2 clinical trial
data, provide evidence of the benefits of deucrictibant as a
potential treatment for HAE, and highlight the importance of
additional data from late-stage clinical development of
deucrictibant in both treatment settings.”
Prophylactic ProgramCHAPTER-1 (NCT05047185) is
a two-part Phase 2 study evaluating the efficacy and safety of
deucrictibant for long-term prophylaxis of HAE attacks. Positive
top-line data from the double-blind, randomized, placebo-controlled
portion (part 1) of the CHAPTER-1 study were announced in December
2023. Further exploration of disease control, health-related
quality of life (HRQoL), and treatment satisfaction data will be
presented by Dr. Markus Magerl in an oral presentation and show
that 90% of participants receiving deucrictibant (N=20) reported
well-controlled HAE at week 12 compared to 37.5% of participants
receiving placebo (N=8) as measured by the Angioedema Control Test
(AECT). Deucrictibant-treated participants reported greater
satisfaction than those treated with placebo with regards to
effectiveness and the domain of global satisfaction, and a
comparable satisfaction for side effects.
All eligible participants completing part 1 of CHAPTER-1 (N=30)
enrolled into the ongoing open-label extension (part 2) during
which they have received deucrictibant 40 mg/day with a mean
treatment duration in the extension of 12.83 months. The current
analysis (cutoff date: June 10, 2024) will be presented by Dr.
Riedl in a poster presentation and show that deucrictibant was
well-tolerated, with no safety signals observed. Efficacy analyses
show:
- Deucrictibant reduced the attack rate in the open-label
extension by 93.0% compared to the part 1 study baseline
- The occurrence of “moderate and severe” attacks and of attacks
treated with on-demand medication remained low in the open-label
extension
On-Demand ProgramDr. Emel Aygören-Pürsün will
present a poster on RAPIDe-2 (NCT05396105), an ongoing two-part
Phase 2/3 extension study, evaluating long-term safety and efficacy
of orally administered deucrictibant immediate-release capsule for
the on-demand treatment of HAE attacks. The safety analysis (cutoff
date: June 10, 2024) includes a total of 337 attacks and shows that
deucrictibant was well-tolerated for all studied doses with no new
safety signals observed. The efficacy analysis (cutoff date: March
1, 2024) includes a total of 265 attacks and shows:
- Median time to onset of symptom relief was 1.1 (PGI-C) hours
with 98.5% of attacks achieving onset of symptom relief by 12
hours
- Median time to reduction in attack severity was 2.6 hours
(PGI-S) with 97.7% of attacks achieving reduction in attack
severity by 12 hours
- Median time to complete attack resolution was 11.5 hours with
85.8% of attacks achieving complete attack resolution within 24
hours (PGI-S) and 90.2% of these attacks requiring a single dose of
deucrictibant
RAPIDe-2 data were used to conduct a comparison of deucrictibant
immediate-release capsule to standard of care on-demand therapy in
a propensity-score matched analysis. The analysis to be presented
by Dr. Riedl in a poster presentation, indicates that PGI-C- and
PGI-S-based outcomes were more favorable for the attacks treated
with deucrictibant in RAPIDe-2 study than for the attacks treated
with standard of care in an observational study.
SafetyDr. Nieves Crespo will present a poster
on an assessment of the cardiovascular safety of deucrictibant
after repeated dosing which shows no evidence of impact on
cardiovascular parameters in nonclinical studies in non-human
primates, including a 3-month and chronic study, nor in clinical
studies to date, following prophylactic treatment up to 12 weeks of
administration in the randomized, placebo-controlled part 1 of
CHAPTER-1 clinical study and up to one year of mean duration
of treatment in its ongoing open-label extension.
The presentation slides and posters are available on the
Investors section of the Pharvaris website
at: https://ir.pharvaris.com/news-events/events-presentations.
About DeucrictibantDeucrictibant is a novel,
potent, oral small-molecule bradykinin B2 receptor antagonist. By
inhibiting bradykinin signaling through the bradykinin B2 receptor,
deucrictibant has the potential to prevent the occurrence of HAE
attacks and to treat the manifestations of an attack if they occur.
Based on its chemical properties, Pharvaris is developing two
formulations of deucrictibant for oral administration: an
extended-release tablet to enable sustained absorption and efficacy
for prophylactic treatment, and an immediate-release capsule to
enable rapid onset of activity for on-demand treatment.
About PharvarisPharvaris is a late-stage
biopharmaceutical company developing novel, oral bradykinin B2
receptor antagonists to prevent and treat HAE attacks. By directly
pursuing this clinically proven therapeutic target with novel small
molecules, the Pharvaris team aspires to offer people with all
types of bradykinin-mediated angioedema effective, well-tolerated,
and easy-to-administer alternatives to treat attacks, both
prophylactically and on-demand. With positive data in both Phase 2
prophylaxis and on-demand studies in HAE, Pharvaris is encouraged
to further develop deucrictibant. Pharvaris is currently enrolling
a pivotal Phase 3 study for the on-demand treatment of HAE attacks
and plans to initiate a pivotal Phase 3 study of deucrictibant for
the prevention of HAE attacks in the coming months. For more
information, visit https://pharvaris.com/.
Forward-Looking StatementsThis press release
contains certain forward-looking statements that involve
substantial risks and uncertainties. All statements contained in
this press release that do not relate to matters of historical fact
should be considered forward-looking statements, including, without
limitation, statements relating to our future plans, studies and
trials, and any statements containing the words “believe,”
“anticipate,” “expect,” “estimate,” “may,” “could,” “should,”
“would,” “will,” “intend” and similar expressions. These
forward-looking statements are based on management’s current
expectations, are neither promises nor guarantees, and involve
known and unknown risks, uncertainties and other important factors
that may cause Pharvaris’ actual results, performance or
achievements to be materially different from its expectations
expressed or implied by the forward-looking statements. Such risks
include but are not limited to the following: uncertainty in the
outcome of our interactions with regulatory authorities, including
the FDA; the expected timing, progress, or success of our clinical
development programs, especially for deucrictibant
immediate-release capsules and deucrictibant extended-release
tablets, which are in late-stage global clinical trials; our
ability to replicate the efficacy and safety demonstrated in the
RAPIDe-1, RAPIDe-2, and CHAPTER-1 Phase 2 studies in ongoing and
future nonclinical studies and clinical trials; risks arising from
epidemic diseases, such as the COVID-19 pandemic, which may
adversely impact our business, nonclinical studies, and clinical
trials; the outcome and timing of regulatory approvals; the value
of our ordinary shares; the timing, costs and other limitations
involved in obtaining regulatory approval for our product
candidates, or any other product candidate that we may develop in
the future; our ability to establish commercial capabilities or
enter into agreements with third parties to market, sell, and
distribute our product candidates; our ability to compete in the
pharmaceutical industry, including with respect to existing
therapies, emerging potentially competitive therapies and with
competitive generic products; our ability to market, commercialize
and achieve market acceptance for our product candidates; our
ability to raise capital when needed and on acceptable terms;
regulatory developments in the United States, the European Union
and other jurisdictions; our ability to protect our intellectual
property and know-how and operate our business without infringing
the intellectual property rights or regulatory exclusivity of
others; our ability to manage negative consequences from changes in
applicable laws and regulations, including tax laws, our ability to
successfully remediate the material weaknesses in our internal
control over financial reporting and to maintain an effective
system of internal control over financial reporting; changes and
uncertainty in general market, political and economic conditions,
including as a result of inflation and the current conflict between
Russia and Ukraine and the Hamas attack against Israel and the
ensuing war; and the other factors described under the headings
“Cautionary Statement Regarding Forward-Looking Statements” and
“Item 3. Key Information—D. Risk Factors” in our Annual Report on
Form 20-F and other periodic filings with the U.S. Securities and
Exchange Commission. These and other important factors could cause
actual results to differ materially from those indicated by the
forward-looking statements made in this press release. Any such
forward-looking statements represent management’s estimates as of
the date of this press release. New risks and uncertainties may
emerge from time to time, and it is not possible to predict all
risks and uncertainties. While Pharvaris may elect to update such
forward-looking statements at some point in the future, Pharvaris
disclaims any obligation to do so, even if subsequent events cause
its views to change. These forward-looking statements should not be
relied upon as representing Pharvaris’ views as of any date
subsequent to the date of this press release.
Contact
Maggie Beller
Executive Director, Head of Corporate and Investor Communications
maggie.beller@pharvaris.com
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