Now Approved for Children of All Ages with
CLN2 Batten Disease, Regardless of Whether They Yet Show
Symptoms
SAN
RAFAEL, Calif., July 24,
2024 /PRNewswire/ -- BioMarin Pharmaceutical Inc.
(Nasdaq: BMRN) today announced that the U.S. Food and Drug
Administration (FDA) has approved the company's supplemental
Biologics License Application (sBLA) for BRINEURA®
(cerliponase alfa) to slow the loss of ambulation in children of
all ages with neuronal ceroid lipofuscinosis type 2 (CLN2 disease),
also known as tripeptidyl peptidase 1 (TPP1) deficiency.
Previously, BRINEURA was indicated in symptomatic children 3 years
of age and older with late infantile CLN2 disease. This expanded
indication now includes children of all ages with CLN2 disease,
regardless of whether they are symptomatic or presymptomatic.
"Today's approval represents a significant step forward in
enabling children to be treated with BRINEURA as early as possible,
when we can have the greatest impact in altering the natural course
of disease," said Hank Fuchs, M.D.,
president of Worldwide Research and Development at BioMarin. "We
know that every day counts for families affected by serious genetic
conditions such as CLN2 disease, which is characterized by a rapid
onset of neurodegenerative symptoms. We have been working
diligently since BRINEURA's initial approval to support this
expanded use in children of all ages, even before they begin to
show symptoms."
The sBLA is supported by data from Study 190-203, a Phase 2,
open-label, multicenter trial evaluating BRINEURA treatment over
the span of approximately three years in children aged 1-6 years at
baseline, including eight children less than 3 years of age.
Results from Study 190-203, which were presented at the 20th Annual
We're Organizing Research on Lysosomal Diseases meeting
(WORLDSymposium) in February, showed that intraventricular
(intracerebroventricular, ICV)-administered BRINEURA slowed the
decline in motor function and delayed disease onset in children
with CLN2 disease, including those who were under 3 years of age.
BRINEURA's safety profile has been well-characterized, and safety
results in children under 3 years of age were similar to the known
safety profile of the medicine. In addition to confirming that
treatment initiated after 3 years of age significantly slows the
progression of CLN2 disease, these are the first data to
demonstrate that early treatment initiation before 3 years of age
may result in delaying disease onset.
In Study 190-203, children were assessed for decline in the
motor domain of the CLN2 Clinical Rating Scale. This domain
measures ambulation, with normal function being a score of three
and no function being a score of zero. Decline was defined as
having a sustained two-point loss or an unreversed score of zero.
In the children below 3 years of age treated with BRINEURA in the
trial, none (0%) had a two-point decline or score of zero in the
motor score by the final assessment (week 169). Among the eight
treated children, seven were matched to 18 untreated children from
a natural history cohort. Among the matched natural history
comparators, 11 children (61%) experienced an unreversed two-point
decline or score of zero by the final assessment. From baseline to
final assessment, all seven matched BRINEURA-treated children below
3 years of age maintained a motor score of three, which represents
a grossly normal gait, signifying a delay in disease onset.
"Receiving a CLN2 diagnosis is devastating for families as the
disease is life-limiting and can severely impact a child's daily
functioning and quality of life from a very young age, with
symptoms including seizures, speech and language deficits, impaired
movement and vision loss," said Ineka
Whiteman, Ph.D., head of Research and Medical Affairs at the
Batten Disease Support, Research, & Advocacy (BDSRA)
Foundation. "The opportunity to start BRINEURA treatment earlier,
even before the onset of symptoms, provides newfound hope for the
families impacted by this rapidly progressive disease. Importantly,
this expanded indication provides further impetus for early
diagnosis of CLN2 disease, as we continue advocating for inclusion
of CLN2 disease on the RUSP (Recommended Uniform Screening Panel)
for newborn screening."
About CLN2 Disease
Children with neuronal ceroid lipofuscinosis type 2 (CLN2
disease), also known as tripeptidyl peptidase 1 (TPP1) deficiency,
typically begin experiencing seizures between the ages of 2 and 4
years old, preceded in the majority of cases by language
development delay. The disease progresses rapidly with most
affected children losing the ability to walk and talk by
approximately 6 years of age. Initial symptoms are followed by
movement disorders, motor deterioration, dementia, blindness, and
death usually occurring between the ages of 8 and 12 years of age.
During the later stages of the disease, feeding and tending to
everyday needs become very difficult. BioMarin estimates the
incidence of CLN2 disease is approximately one in 200,000, with up
to 1,200 to 1,600 children in the regions of the world where
BioMarin operates, many of whom are undiagnosed.
The neuronal ceroid lipofuscinoses (NCLs) are a heterogeneous
group of lysosomal storage disorders that includes the autosomal
recessive neurodegenerative disorder CLN2 disease. CLN2 disease is
caused by mutations in the TPP1 gene resulting in deficient
activity of the enzyme TPP1. In the absence of TPP1, lysosomal
storage materials normally metabolized by this enzyme accumulate in
many organs, particularly in the brain and retina. Buildup of these
storage materials in the cells of the nervous system contributes to
the progressive and relentless neurodegeneration, which manifests
as loss of cognitive, motor and visual functions.
About BRINEURA
BRINEURA is an enzyme replacement therapy indicated to slow the
loss of the ability to walk or crawl (ambulation) in pediatric
patients with neuronal ceroid lipofuscinosis type 2 (CLN2 disease),
also known as tripeptidyl peptidase 1 (TPP1) deficiency, a form of
Batten disease.
BRINEURA is a recombinant form of human TPP1, the enzyme
deficient in children with CLN2 disease, designed to restore TPP1
enzyme activity and break down the storage materials that cause
CLN2 disease. To reach the cells of the brain and central nervous
system, the treatment is delivered directly into the fluid
surrounding the brain (cerebrospinal fluid) using BioMarin's
patented technology.
BRINEURA, the first and only approved treatment for children
with CLN2 disease, was initially approved in 2017 by the U.S. Food
and Drug Administration and European Commission.
Patient Support Accessing BRINEURA
To reach a BioMarin RareConnections® Case Manager,
please call, toll-free, 1-866-906-6100 or e-mail
support@biomarin-rareconnections.com. For more information about
BRINEURA, please visit www.brineura.com. For additional information
regarding this product, please contact BioMarin Medical Information
at medinfo@bmrn.com.
BRINEURA U.S. Important Safety Information
BRINEURA (cerliponase alfa) is a prescription medication used to
slow the loss of ability to walk or crawl (ambulation) in pediatric
patients with neuronal ceroid lipofuscinosis type 2 (CLN2
disease), also known as tripeptidyl peptidase 1 (TPP1)
deficiency.
What is the most important safety information I should know
about BRINEURA?
Severe and life-threatening allergic reactions, including
anaphylaxis, can occur during BRINEURA infusions and up to 24 hours
after infusion. These reactions can occur in people receiving
BRINEURA for the first time or in people who have previously
received BRINEURA without having an allergic reaction.
Your child's doctor will tell you about the symptoms of
life-threatening hypersensitivity reactions, including anaphylaxis
and when to seek immediate medical care. If a severe allergic
reaction (e.g., anaphylaxis) occurs during infusion, the infusion
should be stopped immediately, and your child should receive
medical attention. Contact your doctor or get medical help right
away if your child develops any severe symptoms after infusion.
If anaphylaxis occurs, you and your child's healthcare providers
should consider the risks and benefits of readministration of
BRINEURA. If the decision is made to readminister BRINEURA after
the occurrence of anaphylaxis, the healthcare providers should
ensure appropriately trained personnel and equipment for emergency
resuscitation (including epinephrine and other emergency medicines)
are readily available during infusion and will start the subsequent
infusion at approximately one-half the initial infusion rate at
which the anaphylactic reaction occurred.
Who should not take BRINEURA?
- Patients with active intraventricular access device-related
complications (e.g., leakage, device failure, or device-related
infection, including meningitis)
- Patients with any sign or symptom of acute or unresolved
localized infection around the device insertion site (e.g.,
cellulitis or abscess) or suspected or confirmed central nervous
system (CNS) infection (e.g., cloudy cerebrospinal fluid [CSF] or
positive CSF gram stain, or meningitis)
- Patients with shunts used to drain extra fluid around the
brain
Administration: BRINEURA is only given by infusion
into the fluid of the brain (known as an intraventricular infusion)
and using sterile technique to reduce the risk of infection. An
intraventricular access device or port must be in place at least 5
to 7 days prior to the first infusion.
- Prior to administration, it is important to discuss your
child's medical history with their doctor
- Tell the doctor if they are sick or taking any medication and
if they are allergic to any medicines
Meningitis and other device-related
infections: Intraventricular access device-related
infections, including meningitis, were observed with BRINEURA
treatment. Infections required treatment with antibiotics and
removal of the access device. If any signs of infection or
meningitis occur, contact your child's doctor immediately. The
signs and symptoms of infections may not be readily apparent in
patients with CLN2 disease.
- Your child's doctor should vigilantly be looking for signs and
symptoms of infection, including meningitis, during treatment with
BRINEURA
- Your child's doctor should inspect the scalp and collect
samples of your child's CSF prior to each infusion of BRINEURA, to
check for infections and that there is no device failure
- Signs of infection on or around the device insertion site may
include redness, tenderness, or discharge
Device-related complications such as device leakage,
device failure, extravasation of CSF fluid, or bulging of the scalp
around or above the intraventricular access device have occurred.
In case of intraventricular access device-related complications,
BRINEURA infusions may be discontinued.
Material degradation of the intraventricular access device
reservoir was reported after approximately 4 years of
administration, which may impact the effective and safe use of the
device. During testing such material degradation was recognized
after approximately 105 perforations of the intraventricular access
device. The intraventricular access device should be replaced prior
to 4 years of single-puncture administrations, which equates to
approximately 105 administrations of BRINEURA.
Cardiovascular side effects: Low blood pressure
and/or slow heart rate may occur during and following the infusion
of BRINEURA. Contact your child's healthcare provider immediately
if these reactions occur. As part of the infusion, the healthcare
provider will monitor vital signs (blood pressure, heart rate)
before infusion starts, periodically during infusion, and
post-infusion, and assess the patient's status after administration
to determine if continued observation may be necessary. Additional
monitoring is required for patients with a history of cardiac
abnormalities. In patients without cardiac abnormalities, regular
12-lead electrocardiogram (ECG) evaluations should be performed
every 6 months.
Infusion-associated reactions (IARs) such as vomiting,
seizure, rash, fever (pyrexia), hypersensitivity, and anaphylactic
reaction have been observed in patients treated
with BRINEURA.
Patients less than 37 weeks post-menstrual age (gestational
at birth plus post-natal age) or those weighing less than
2.5kg: BRINEURA is not recommended for use in these patients
due to physiologic immaturity which may increase risk of serious
and clinically significant adverse reactions observed with
BRINEURA.
The most common side effects reported during
BRINEURA infusions included:
- Fever, problems with the electrical activity of the heart,
decreased or increased protein in the fluid of the brain, vomiting,
seizures, device-related complications, hypersensitivity,
collection of blood outside of blood vessels (hematoma), headache,
irritability, increased white blood cell count in the fluid of the
brain, device-related infection, slow heart rate, feeling jittery,
and low blood pressure.
- The most frequent adverse reactions reported in patients < 3
years treated with BRINEURA were similar to those observed in
patients ≥ 3 years of age except for hypersensitivity reactions,
which were reported in 5 of 8 (63%) of patients < 3 years at
baseline compared with 0 of 6 of patients ≥ 3 years of age at
baseline. The most common manifestations of hypersensitivity were
fever (pyrexia) and vomiting and the timing and resolution were
similar to Trials 1 and 2. Symptoms of severe hypersensitivity
reactions (e.g., anaphylaxis) included rapid heart rate
(tachycardia), contraction of the muscles of the airways
(bronchospasm), rash, diarrhea, low blood pressure (hypotension),
increased body temperature and vomiting.
The risk information provided here is not comprehensive. Talk
to your healthcare provider to learn more or for medical advice
about any side effects.
You are encouraged to report negative side effects of
prescription drugs to the FDA. Visit www.fda.gov/medwatch or call
1-800-FDA-1088.
Please click here to see full Prescribing Information
or visit www.brineura.com.
About BioMarin
Founded in 1997, BioMarin is a global biotechnology company
dedicated to transforming lives through genetic discovery. The
company develops and commercializes targeted therapies that address
the root cause of genetic conditions. BioMarin's unparalleled
research and development capabilities have resulted in eight
transformational commercial therapies for patients with rare
genetic disorders. The company's distinctive approach to drug
discovery has produced a diverse pipeline of commercial, clinical,
and pre-clinical candidates that address a significant unmet
medical need, have well-understood biology, and provide an
opportunity to be first-to-market or offer a substantial benefit
over existing treatment options. For additional information, please
visit www.biomarin.com.
Forward-Looking Statements
This press release contains forward-looking statements about the
business prospects of BioMarin Pharmaceutical Inc. (BioMarin),
including without limitation, statements about: the impact of the
U.S. Food and Drug Administration (FDA) approval of the
supplemental Biologics License Application for BRINEURA to
slow the loss of ambulation in children of all ages with neuronal
ceroid lipofuscinosis type 2 (CLN2 disease), also known as
tripeptidyl peptidase 1 (TPP1) deficiency, including the ability to
alter the natural course of the disease through early treatment.
These forward-looking statements are predictions and involve risks
and uncertainties such that actual results may differ materially
from these statements. These risks and uncertainties include, among
others: results and timing of current and planned preclinical
studies and clinical trials of BRINEURA; any potential adverse
events observed in the continuing monitoring of the patients in the
clinical trials; the content and timing of decisions by regulatory
agencies other than the FDA; and those factors detailed in
BioMarin's filings with the Securities and Exchange Commission,
including, without limitation, the factors contained under the
caption "Risk Factors" in BioMarin's Quarterly Report on Form 10-Q
for the quarter ended March 31, 2024,
as such factors may be updated by any subsequent reports.
Stockholders are urged not to place undue reliance on
forward-looking statements, which speak only as of the date hereof.
BioMarin is under no obligation, and expressly disclaims any
obligation to update or alter any forward-looking statement,
whether as a result of new information, future events or
otherwise.
BioMarin®, BioMarin RareConnections®
and BRINEURA® are registered trademarks of BioMarin
Pharmaceutical Inc.
Contacts:
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Investors
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Media
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Traci McCarty
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Andrew Villani
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BioMarin
Pharmaceutical Inc.
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BioMarin
Pharmaceutical Inc.
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(415)
455-7558
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(628)
269-7393
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SOURCE BioMarin Pharmaceutical Inc.