BioCryst Pharmaceuticals, Inc. (Nasdaq: BCRX) today announced
new real-world comparative research on the use of oral, once-daily
ORLADEYO® (berotralstat) that found high rates of adherence and
persistence for ORLADEYO, similar to the rates observed with two
other long-term prophylactic (LTP) therapies for hereditary
angioedema (HAE).
The company also announced new real-world
evidence showing statistically significant and sustained HAE attack
rate reductions after initiating ORLADEYO in patients with HAE,
regardless of their C1-inhibitor (C1-INH) deficiency status, and
new findings from an HAE patient survey confirming patient
preference for an oral LTP therapy.
“These results build on previous research that
highlights how the real-world effectiveness and convenience of our
oral, once-daily prophylactic therapy are differentiators for
patients. The strong adherence, persistence and preference for
ORLADEYO we report here provide further evidence that enables
physicians to optimize individualized treatment recommendations for
each of their patients. We continue to generate real-world evidence
demonstrating that ORLADEYO is a powerful, potentially
life-changing treatment for many people with HAE,” said Dr. Donald
S. Fong, chief medical officer of BioCryst.
The data are being presented at the Annual
Scientific Meeting of the American College of Allergy, Asthma &
Immunology (ACAAI), which is taking place in Boston from October
24-28, 2024.
High Adherence and Persistence Rates for
ORLADEYO and Other LTP Therapies
Poster #R072 explores adherence and persistence
rates among patients with HAE following initiation of ORLADEYO
(n=90) compared with lanadelumab (n=189) and subcutaneous
plasma-derived C1-inhibitor (SC-pdC1-INH) (n=78).
“Our findings reveal that among HAE patients
managed with LTP, high adherence and persistence rates were
demonstrated for ORLADEYO. There was a striking consistency between
first line therapies with comparable results for lanadelumab and
SC-pdC1-INH. ORLADEYO rates were equivalent to – and in some cases
better than – these LTP counterparts. The outcomes of our study
provide further support for a shared decision-making approach
within the physician-patient partnership to inform LTP selection,
incorporating effectiveness, safety, treatment burden and patient
preference for each individual,” said Sandra Christiansen, MD,
professor of medicine and director of translational research at the
US HAEA Angioedema Center at the University of California, San
Diego.
- Adherence And Persistence
Among Hereditary Angioedema Patients Treated With Berotralstat,
Lanadelumab, And Subcutaneous Plasma-Derived C1-Inhibitor;
ePoster #R072; Friday, October 25, 2:30-2:45 p.m. ET; Monitor #19,
Hall A
- Eighty-six percent of patients who
took ORLADEYO (n=77), 91 percent who took lanadelumab (n=172) and
83 percent who took SC-pdC1-INH (n=65) filled at least two
prescriptions during the 12-month follow-up period.
- Adherence rates among patients with
at least two fills were high at 12 months of
follow-up. Seventy-seven percent of patients taking ORLADEYO
were adherent compared to 76 percent of patients taking lanadelumab
and 80 percent of patients taking SC-pdC1-INH.
- Persistence rates among patients with at least two fills were
high at 12 months of follow-up, with 71 percent of patients taking
ORLADEYO persistent compared to 63 percent of patients taking
lanadelumab and 63 percent of patients taking SC-pdC1-INH.
- No statistically significant differences in adherence or
persistence were observed between the LTP patient cohorts.
Methods
- Electronic health records linked to
claims data were used to select mutually exclusive cohorts of
patients aged 12 and above who initiated ORLADEYO, lanadelumab or
pdC1-INH between June 22, 2017, and September 12, 2023.
- Adherence was defined as having a
proportion of days covered greater than or equal to 0.80.
- Persistence was defined as fewer
than 45 consecutive days without the index LTP treatment.
Sustained HAE Attack Rate Reduction After
Beginning ORLADEYO Regardless of C1-INH Status
Posters #R092 and #R093 evaluate self-reported
HAE attacks prior to and following ORLADEYO initiation among
patients with and without HAE with C1-inhibitor deficiency
(HAE-nl-C1-INH), respectively.
“ORLADEYO was associated with statistically
significant and sustained reductions in attack rates through 18
months (540 days) following ORLADEYO initiation, regardless of
patients’ C1-INH status. Importantly, in this real-world study,
patients with zero attacks at baseline were included, compared to
the minimum of two attacks that was required at baseline in APeX-2.
These data confirm that many already well-controlled HAE patients
enjoy continued or improved attack control once they initiate
ORLADEYO,” Dr. Fong added.
- Sustained Real-World Attack
Reductions Following Berotralstat Initiation Among Patients with
Hereditary Angioedema with C1-Inhibitor Deficiency;
ePoster #R092; Friday, October 25, 3:30-3:45 p.m. ET; Monitor #20,
Hall A
- Patients (n=466) had significantly
lower attack rates at each follow-up interval, which ranged from
0.62 attacks per month at days 361-450 (n=185) to 0.79 at days
271-360 (n=217) versus baseline (2.62 at days 361-450 to 2.50 at
days 271-360).
- Mean monthly attack rate reduction
was -1.71 (p<0.05) at days 271-360 (n=217) and -1.96 (p<0.05)
at days 451-540 (n=157).
- Sustained Real-World Attack
Reductions Following Berotralstat Initiation Among Patients with
Hereditary Angioedema without C1-Inhibitor Deficiency;
ePoster #R093; Friday, October 25, 3:45-4:00 p.m. ET; Monitor #20,
Hall A
- Patients (n=353) had significantly
lower attack rates at each follow-up interval, which ranged from
1.63 attacks per month at days 181-270 (n=191) to 2.04 at days 1-90
(n=304) versus baseline (4.33 at days 181-270 to 4.63 at days
1-90).
- Mean monthly attack rate reduction
was -2.91 (p<0.05) at days 271-360 (n=157) and -2.53 (p<0.05)
at days 451-540 (n=108).
Methods
- Outcomes were collected through
BioCryst’s sole-source pharmacy and included U.S. patients who
actively received ORLADEYO 110 or 150 mg QD from December 15, 2020,
to January 8, 2024.
- Patient-reported HAE attack rates
were collected at baseline and each refill (approximately every 30
days).
- To be included in the analysis of a
given follow-up period, patients were required to have responded to
a follow-up assessment within the period of interest and to the
onboarding self-assessment of attacks. Approximately 96 percent of
patients met these criteria at each interval.
Patients with HAE Prefer Oral LTP
Poster #R081 examines the LTP treatment
preferences of patients with HAE, as collected through an online
survey.
“We are encouraged to see both effectiveness and
convenience are drivers of treatment preference with patients
preferring oral therapy over injectable therapy when efficacy is
assumed equal. Given the benefits of treatment with ORLADEYO for
patients who remain on therapy over the long term, we believe we
will continue to see the preference towards oral therapy reflected
in the strong commercial performance of our oral, once-daily
prophylactic therapy for HAE,” Dr. Fong noted.
- Long-Term Prophylactic
Treatment Preferences of Patients With Hereditary
Angioedema; ePoster #R081; Friday, October 25, 4:45-5:00
p.m. ET; Monitor #19, Hall A
- LTP treatment attributes rated most
important were effectiveness in attack prevention and effectiveness
in reducing attack severity.
- When presented with the option of
an equally effective oral or injectable LTP, 54 percent preferred
an oral daily therapy over a biweekly or monthly subcutaneous
injection.
- More than half (52 percent)
preferred oral over injectable LTP as infrequently as every three
months.
Methods
- Results from an online survey of
U.S. patients with HAE who were at least 18 years of age,
self-reported their diagnosis and were receiving an HAE treatment
(LTP, on-demand or both) or had experienced at least one HAE attack
in the preceding three months (n=150).
In addition to displaying in the exhibit hall at
the noted times, ePosters are accessible online and on demand to
registered attendees on ACAAI’s website.
About
ORLADEYO® (berotralstat)ORLADEYO® (berotralstat)
is the first and only oral therapy designed specifically to prevent
attacks of hereditary angioedema (HAE) in adult and pediatric
patients 12 years and older. One capsule of ORLADEYO per day works
to prevent HAE attacks by decreasing the activity of plasma
kallikrein.
U.S. Indication and Important Safety
Information
INDICATIONORLADEYO® (berotralstat) is a
plasma kallikrein inhibitor indicated for prophylaxis to prevent
attacks of hereditary angioedema (HAE) in adults and pediatric
patients 12 years and older.
Limitations of useThe safety
and effectiveness of ORLADEYO for the treatment of acute HAE
attacks have not been established. ORLADEYO should not be used for
the treatment of acute HAE attacks. Additional doses or dosages of
ORLADEYO higher than 150 mg once daily are not recommended due to
the potential for QT prolongation.
IMPORTANT SAFETY INFORMATION
An increase in QT prolongation was observed at
dosages higher than the recommended 150 mg once-daily dosage and
was concentration dependent.
The most common adverse reactions (≥10% and
higher than placebo) in patients receiving ORLADEYO were abdominal
pain, vomiting, diarrhea, back pain, and gastroesophageal reflux
disease.
A reduced dosage of 110 mg taken orally once
daily with food is recommended in patients with moderate or severe
hepatic impairment (Child-Pugh B or C).
Berotralstat is a substrate of P-glycoprotein
(P-gp) and breast cancer resistance protein. P-gp inducers (eg,
rifampin, St. John’s wort) may decrease berotralstat plasma
concentration, leading to reduced efficacy of ORLADEYO. The use of
P-gp inducers is not recommended with ORLADEYO.
ORLADEYO at a dose of 150 mg is a moderate
inhibitor of CYP2D6 and CYP3A4. For concomitant medications with a
narrow therapeutic index that are predominantly metabolized by
CYP2D6 or CYP3A4, appropriate monitoring and dose titration is
recommended. ORLADEYO at a dose of 300 mg is a P-gp inhibitor.
Appropriate monitoring and dose titration is recommended for P-gp
substrates (eg, digoxin) when coadministering with ORLADEYO.
The safety and effectiveness of ORLADEYO in
pediatric patients <12 years of age have not been
established.
There are insufficient data available to inform
drug-related risks with ORLADEYO use in pregnancy. There are no
data on the presence of berotralstat in human milk, its effects on
the breastfed infant, or its effects on milk production.
To report SUSPECTED ADVERSE REACTIONS,
contact BioCryst Pharmaceuticals, Inc. at 1-833-633-2279 or FDA at
1-800-FDA-1088
or www.fda.gov/medwatch.
Please see
full Prescribing
Information.
About BioCryst Pharmaceuticals
BioCryst Pharmaceuticals is a global biotechnology company with a
deep commitment to improving the lives of people living with
complement-mediated and other rare diseases. BioCryst leverages its
expertise in structure-guided drug design to develop first-in-class
or best-in-class oral small-molecule and protein therapeutics to
target difficult-to-treat diseases. BioCryst has commercialized
ORLADEYO® (berotralstat), the first oral, once-daily plasma
kallikrein inhibitor, and is advancing a pipeline of small-molecule
and protein therapies. For more information, please visit
www.biocryst.com or follow us on LinkedIn.
Forward-Looking Statements
This press release contains forward-looking
statements, including statements regarding future results,
performance or achievements and statements relating to ORLADEYO
performance and patient preferences. These statements involve known
and unknown risks, uncertainties and other factors which may cause
actual results, performance or achievements to be materially
different from any future results, performance or achievements
expressed or implied by the forward-looking statements. These
statements reflect our current views with respect to future events
and are based on assumptions and are subject to risks and
uncertainties. Given these uncertainties, you should not place
undue reliance on these forward-looking statements. Some of the
factors that could affect the forward-looking statements contained
herein include: BioCryst’s ability to successfully implement or
maintain its commercialization plans for ORLADEYO, which could take
longer or be more expensive than planned; the commercial viability
of ORLADEYO, including its ability to achieve sustained market
acceptance; the FDA or other applicable regulatory agency may
require additional studies beyond the studies planned for products
and product candidates, may not provide regulatory clearances which
may result in delay of planned clinical trials, may impose certain
restrictions, warnings, or other requirements on products and
product candidates, may impose a clinical hold with respect to
product candidates, or may withhold, delay, or withdraw market
approval for products and product candidates; BioCryst’s ability to
successfully manage its growth and compete effectively; and risks
related to the international expansion of BioCryst’s business.
Please refer to the documents BioCryst files periodically with the
Securities and Exchange Commission, specifically BioCryst’s most
recent Annual Report on Form 10-K, Quarterly Reports on Form 10-Q,
and Current Reports on Form 8-K, which identify important factors
that could cause the actual results to differ materially from those
contained in BioCryst’s forward-looking statements.
BCRXW
Contact:John Bluth+1 919 859
7910jbluth@biocryst.com
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