NAARDEN, Netherlands & WALTHAM,
Mass.--(BUSINESS WIRE)-- Prilenia Therapeutics B.V., a biopharmaceutical company focused on
developing novel therapeutics to treat neurodegenerative and neurodevelopmental diseases, today announced
the presentation of five scientific abstracts and an oral presentation focused on pridopidine, the company’s
investigational medicine for the treatment of Huntington’s disease (HD), at the upcoming 31 st
annual meeting of the Huntington Study Group to be held in Cincinnati, Ohio, November 7-9, 2024.
“To provide truly meaningful change for people living with HD, we need to shift
the paradigm from treating symptoms to addressing progression. The data we will present at HSG reinforce
pridopidine’s benefits across function, cognition and fine motor skills measured by validated assessments
and sustained for up to two years,” said Dr. Michael R. Hayden, Chief Executive Officer of Prilenia. “The
European Medicines Agency has accepted our MAA submission for the treatment of HD, and it is currently under
review. This is the first submission seeking approval for a potentially first-in-class investigational new
treatment that can impact these measures of clinical disease progression in HD.”
Dr. Hayden will present clinical data on pridopidine during the Contemporary
Trials and Next Steps (Clinical Trial Roundup) session (10:45–12:15 ET, Friday, November 8), additional to
presentation of the five abstracts. The data demonstrate pridopidine’s effect and implications for HD
management and clinical trial design:
- The Phase 3 PROOF-HD Trial Demonstrates
Significant Benefits of Pridopidine on Progression, Cognition, and Motor Function in Huntington’s
Disease
- Overview:
Pridopidine shows consistent, sustained, and clinically meaningful benefits across multiple
endpoints, including function, clinical disease progression (as measured by cUHDRS), cognition,
motor and quality of life in patients not receiving antidopaminergics (ADMs) and on low doses of
ADMs.
- Integrated Efficacy Analysis of Four
Randomized Placebo-Controlled Trials Supports Pridopidine’s Treatment Benefits Across Key Clinical
Measures of Huntington’s Disease
- Overview:
The integrated efficacy analysis from four clinical trials supports PROOF-HD findings, showing
consistent, sustained and clinically meaningful benefits of pridopidine in HD in patients not
receiving ADMs.
- Pridopidine Demonstrates Consistent
Improvements in Q-Motor Measures, and Early Benefits in Q-Motor Predict Long-Term Changes in
Function and cUHDRS in PROOF-HD
- Overview:
Pridopidine demonstrated improvements in Q-Motor assessments at all timepoints irrespective of
ADM use, with strongest and most significant effects in patients not receiving ADMs. Early
improvements in Q-Motor were predictive of long-term benefits on key clinical outcome measures
of disease progression.
- Low Dose Antidopaminergic Medications do not
Mask the Beneficial Effects of Pridopidine in Huntington’s Disease
- Overview: Participants on
low dose ADMs maintain the positive and clinically meaningful benefits of pridopidine in HD.
These observations may guide the use of ADMs for the treatment of chorea and behavioral
disorders together with pridopidine.
- The Effect of Antidopaminergic Medications
on Huntington’s Disease
- Overview: Analyses of data
from the ENROLL-HD database demonstrate that use of ADM’s was associated with worse outcomes in
clinical outcome measures typically used in HD for function, cognition, cUHDRS and motor
performance. These observations have important implications for the conduct and interpretation
of investigational studies of disease-modifying agents in HD and for medical practice.
About Pridopidine
Pridopidine (45 mg twice daily) is a potent and highly selective, orally
administered, sigma-1 receptor (S1R) agonist, that has the potential to alter treatment paradigms in
neurodegenerative diseases. S1R regulates several cellular neuroprotective mechanisms commonly impaired in
neurodegenerative diseases, such as HD and ALS.
Pridopidine has an extensive clinical development program encompassing efficacy
and safety data. In the PROOF-HD Phase 3 clinical trial, pre-specified analyses that excluded patients
receiving antidopaminergics (ADMs) showed benefits in people taking pridopidine across multiple measures,
including clinical disease progression as measured by cUHDRS, cognition (Stroop Word Reading Test, SWR) and
motor (Q-Motor). The primary and secondary endpoints in the full population were not met. Importantly, an
integrated efficacy analysis from four Phase 3 and Phase 2 studies supports and validates the PROOF-HD
findings, showing consistent, sustained and clinically meaningful benefits of pridopidine in HD in patients
not receiving ADMs as measured by cUHDRS (excluding SWR as PRIDE-HD did not measure SWR), Q-Motor Finger
Tapping (FT) and Pronation/Supination (PS).
In clinical studies to date, pridopidine (45 mg twice daily) has been
well-tolerated with a safety and tolerability profile similar to placebo.
The European Medicines Agency has accepted our MAA submission for the treatment of
HD, and it is currently under review. In parallel, Prilenia is also in discussions with the U.S. Food and
Drug Administration (FDA) to determine next steps for HD in the United States. The Company will also
consider regulatory submissions elsewhere globally following the regulatory review process in Europe.
Prilenia holds Orphan Drug designation for pridopidine in HD and ALS in the U.S.
and EU. In addition, pridopidine has received Fast Track designation by the U.S. Food and Drug
Administration (FDA) for the treatment of HD.
About HD
Huntington’s disease (HD) is a rare, inherited, autosomal dominant,
neurodegenerative disease that results in functional, motor, cognitive and behavioral symptoms. HD is caused
by a mutation in the huntingtin gene, and each child of a parent with HD has a 50 percent chance
of developing the disease.
HD affects about 100,000 people around the world with an additional 300,000 people
at risk of developing HD. It is usually diagnosed between the ages of 30 and 50, although HD can occur at
any age, including in children and young adults (known as juvenile onset HD or JHD). The disease progresses
slowly over 15 to 20 years, with patients slowly losing their ability to work, communicate, manage
day-to-day life and take care of themselves. This increasing disability leads to full reliance on a
caregiver and, ultimately, death.
The only currently available treatments for HD focus on symptomatic relief and
palliative care, with nothing impacting measures of overall disease progression.
About Prilenia
Prilenia Therapeutics is a biopharmaceutical company focused on developing novel
therapeutics to treat neurodegenerative and neurodevelopmental diseases like Huntington’s disease (HD) and
amyotrophic lateral sclerosis (ALS). Our team has an unwavering dedication to scientific excellence, and we
are driven by our passion and commitment to patients and their families, caregivers, and communities around
the world affected by these diseases.
Based on the collective data from pridopidine’s extensive development program,
Prilenia is pursuing regulatory approval for its investigational medicine, pridopidine, for the treatment of
HD and planning to initiate a single pivotal Phase 3 study in ALS. Pridopidine is a potent and selective,
orally administered S1R agonist.
Prilenia is a private, Netherlands-headquartered company backed by leading life
sciences investors.
For more information, please visit www.prilenia.com and connect with us on LinkedIn or X (Twitter).
© 2024 Prilenia Therapeutics B.V.
For a copy of this release, visit Prilenia’s website at www.prilenia.com.
Prilenia Contact
Communications Team
info@prilenia.com
Source: Prilenia Therapeutics B.V.