VX15/2503 Treatment for Huntington's Disease
Status: | Active, not recruiting |
---|---|
Conditions: | Neurology |
Therapuetic Areas: | Neurology |
Healthy: | No |
Age Range: | 21 - Any |
Updated: | 2/7/2019 |
Start Date: | July 2015 |
End Date: | May 2020 |
A Phase 2, Multi-center, Randomized, Double-blind, Placebo Controlled Study in Subjects With Late Prodromal and Early Manifest Huntington's Disease (HD) to Assess the Safety, Tolerability, Pharmacokinetics, and Efficacy of VX15/2503
The purpose of this study is to evaluate the safety, tolerability, PK, and efficacy of
VX15/2503 in subjects with late prodromal and early manifest Huntington's disease.
VX15/2503 in subjects with late prodromal and early manifest Huntington's disease.
VX15/2503-N-131 is a Phase 2, multi-center, randomized, double-blind, placebo controlled
study of VX15/2503 in subjects with late prodromal and early manifest Huntington's disease.
The primary objective is to evaluate the safety and tolerability of monthly IV administration
of a single dosage of VX15/2503 (or placebo). Efficacy endpoints include determining the
effect of VX15/2503 on brain volumes (MRI), FDG-PET imaging, 11C-PBR28 (TSPO) PET imaging
(subset of Cohort B only) and clinical features of HD including cognition, motor function,
behavior, functional abilities, global function and global measurement of change. Additional
endpoints include PK / PD, immunogenicity, and exploratory biomarkers. Subjects in Cohort B
that have received 12 months of VX15/2503 who volunteer will undergo a lumbar puncture at V13
to collect cerebral spinal fluid (CSF) to evaluate VX15/2503 mAb concentrations, total
sSEMA4D levels, and other biomarkers in their CSF. Enrollment will involve approximately 276
individuals who are 21 years of age or older with late prodromal (CAG-age product score (CAP
score) of greater than 200 and Diagnostic Confidence Level (DCL) of 2 or 3) or early manifest
HD (Total Functional Capacity (TFC) greater than or equal to 11). The study will be divided
into Cohort A and Cohort B. Cohort A is now complete and an unblinded analysis has been
performed. Cohort A subjects were treated for 6 months with either drug or placebo (1:1) and
then all subjects were treated with drug for 6 months, followed by 3 months of follow up.
Treatment duration for each subject in Cohort A was 12 months. Participation in Cohort A
included a Screening visit, a Baseline visit within 30 days of screening; 12 monthly
treatment visits beginning at baseline and continuing through Month 12; follow-up safety
phone call at one month and a follow-up safety visit three months after the final infusion.
Cohort A subjects participated in the study for approximately 16 months. Based on the
analysis of Cohort A, it was decided to extend the duration of treatment for a subset of
subjects in Cohort B to evaluate the clinical response to VX15/2503 after 36 months.
Additional enrolled subjects in Cohort B will be treated with drug or placebo (1:1).
Participation in Cohort B will include a Screening visit, a Baseline visit within 30 days of
screening; 18 or 36 monthly visits beginning at baseline and continuing through Month 18 or
Month 36; follow-up safety phone call or visit, and for a subset of subjects, a follow-up
safety visit three and six months after the final infusion. Cohort B subjects will
participate in the study for approximately 19 and up to 37 months.
study of VX15/2503 in subjects with late prodromal and early manifest Huntington's disease.
The primary objective is to evaluate the safety and tolerability of monthly IV administration
of a single dosage of VX15/2503 (or placebo). Efficacy endpoints include determining the
effect of VX15/2503 on brain volumes (MRI), FDG-PET imaging, 11C-PBR28 (TSPO) PET imaging
(subset of Cohort B only) and clinical features of HD including cognition, motor function,
behavior, functional abilities, global function and global measurement of change. Additional
endpoints include PK / PD, immunogenicity, and exploratory biomarkers. Subjects in Cohort B
that have received 12 months of VX15/2503 who volunteer will undergo a lumbar puncture at V13
to collect cerebral spinal fluid (CSF) to evaluate VX15/2503 mAb concentrations, total
sSEMA4D levels, and other biomarkers in their CSF. Enrollment will involve approximately 276
individuals who are 21 years of age or older with late prodromal (CAG-age product score (CAP
score) of greater than 200 and Diagnostic Confidence Level (DCL) of 2 or 3) or early manifest
HD (Total Functional Capacity (TFC) greater than or equal to 11). The study will be divided
into Cohort A and Cohort B. Cohort A is now complete and an unblinded analysis has been
performed. Cohort A subjects were treated for 6 months with either drug or placebo (1:1) and
then all subjects were treated with drug for 6 months, followed by 3 months of follow up.
Treatment duration for each subject in Cohort A was 12 months. Participation in Cohort A
included a Screening visit, a Baseline visit within 30 days of screening; 12 monthly
treatment visits beginning at baseline and continuing through Month 12; follow-up safety
phone call at one month and a follow-up safety visit three months after the final infusion.
Cohort A subjects participated in the study for approximately 16 months. Based on the
analysis of Cohort A, it was decided to extend the duration of treatment for a subset of
subjects in Cohort B to evaluate the clinical response to VX15/2503 after 36 months.
Additional enrolled subjects in Cohort B will be treated with drug or placebo (1:1).
Participation in Cohort B will include a Screening visit, a Baseline visit within 30 days of
screening; 18 or 36 monthly visits beginning at baseline and continuing through Month 18 or
Month 36; follow-up safety phone call or visit, and for a subset of subjects, a follow-up
safety visit three and six months after the final infusion. Cohort B subjects will
participate in the study for approximately 19 and up to 37 months.
Inclusion Criteria Highlights:
1. Male or female and are at least greater than or equal to 21 years of age at Screening.
2. Must fulfill one of the following criteria at Screening:
1. Late prodromal HD as defined by a CAP score of greater than 200 and DCL 2 or 3.
2. Early manifest HD as defined by a TFC greater than or equal to 11. Subject must
have been determined to have a clinical diagnosis of HD by the Site Investigator
as defined by a DCL of 4.
3. Must fulfill both of the following criteria at Screening:
1. Have undergone genetic testing with a known CAG repeat greater than or equal to
36.
2. No features of juvenile HD (Westphal variant).
4. If female must be either surgically sterile, postmenopausal, or nonlactating and
nonpregnant. Female subjects of childbearing potential must practice a highly
effective method of contraception.
5. If male, must agree to use a reliable method of birth control (condoms with
contraceptive foams or sexual abstinence) during the study and for 6 months after the
last dose of study drug.
6. Are willing and capable of providing informed consent for study participation, CAG
genotyping (all subjects).
7. Are capable of reading, writing, and communicating effectively with others.
8. Are taking stable doses of any concomitant medications (including tetrabenazine and
deutetrabenazine) during the 1 month prior to the Baseline Visit, with the exception
of newly prescribed anxiolytics for the use of pre-medication prior to imaging at
screening, which will be permitted on a case-by-case basis.
9. Must meet all criteria required to move forward with the Randomization Authorization
Flow (RAF) and be considered eligible by the RAF Reviewer.
Exclusion Criteria Highlights:
1. Have participated in an investigational drug or device study within 30 days of the
Baseline Visit, or 180 days if previous investigational drug was a MAb therapeutic, or
previously participated in SIGNAL Cohort A. This does not apply to Cohort B subjects
who are being offered the option to participate in the extension of Cohort B.
2. Have had previous neurosurgery for Huntington's disease or other movement disorders.
3. Are a suicide risk, as determined by meeting any of the following criteria:
1. suicide attempt within one year prior to Baseline.
2. suicidal ideation as defined by a positive response to question 5 on the C-SSRS
(Baseline visit form) suicidal ideation section, within 60 days of the Baseline
Visit.
3. significant risk of suicide, as judged by the site Investigator.
4. Have marked cognitive impairment with a Montreal Cognitive Assessment (MoCA) Score
less than or equal to 22.
5. Have a presence of clinically significant psychosis and/or confusional states, in the
opinion of the site Investigator.
6. Have clinically significant laboratory or ECG abnormalities at Screening, in the
opinion of the site Investigator.
7. Have clinically relevant hematologic, hepatic, cardiac, or renal disease.
8. Have a medical history of infection with human immunodeficiency virus, hepatitis C
and/or hepatitis B, or found to have an abnormality at Screening.
9. Have a history of substance abuse (based on DSMIV criteria) within the past 12 months
prior to Screening.
10. If female are pregnant or breastfeeding.
11. Have a known allergy to any ingredient in the study drug.
12. Have a history of malignancy of any type within 2 years prior to Screening. A history
of surgically excised non-melanoma skin cancers, and superficial bladder or prostate
cancer is permitted.
13. Have a clinically significant medical, surgical, laboratory, or behavioral abnormality
which in the judgment of the site Investigator makes the subject unsuitable for the
study.
14. Have any significant findings not related to HD on the screening MRI which in the
judgment of the site Investigator makes the subject unsuitable for the study.
15. Have any of the following conditions (which would exclude MRI participation):
1. An implant/device/condition that is contraindicated for MRI (e.g. pacemaker,
severe claustrophobia, prosthetic heart valve, any metal fragments in the eyes or
body--in some cases, an X-ray may be needed before an MRI scan, to ensure it is
safe to enter the scanner).
2. Body habitus that would impede completion of MRI scan. (Subject weight above 158
kg should be discussed with the Medical Monitor).
NOTE: If PET is done on PET-MRI all the above conditions apply for PET-MRI.
16. Are undergoing FDG-PET and have received research-related radiation exposure that
exceeds institutional guidelines in the prior year if applicable.
17. Are undergoing a LP for CSF collection and have any of the following conditions:
uncorrected bleeding or clotting disorders, skin infections near the site of the LP,
suspicion of increased intracranial pressure, allergies to numbing medications (local
anesthetics), acute spinal trauma, history of migraines.
18. Are undergoing a LP for CSF collection and taking any of the following types of
anticoagulants: coumarins and indandiones, Factor Xa inhibitors, heparins, or thrombin
inhibitors.
We found this trial at
29
sites
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Columbia University In 1897, the university moved from Forty-ninth Street and Madison Avenue, where it...
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340 W 10th St #6200
Indianapolis, Indiana 46202
Indianapolis, Indiana 46202
(317) 274-3772
Indiana University School of Medicine With more than 2,000 students in 2013, the Indiana University...
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