Phase 2A Study of GM 608 in Mild to Moderate Parkinson Disease

Parkinson's Disease Clinical Trial

— GAP-PD  

Official title:

GM 608 in A Phase IIA Pilot Double-blinded, Randomized, Placebo Controlled Trial in Mild to Moderate Parkinson Disease

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT01850381
• Other study ID #: GBD 002
• Status: Completed
• Phase: Phase 2
• Start date: June 2013
• Est. completion date: July 2014

Study information

• Verified date: July 2019
• Source: Genervon Biopharmaceuticals, LLC
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

GM608 is an endogenous human embryonic stage neural regulatory and signaling peptide that controls the development, monitoring and correction of the human nervous system. The study drug is an oligopeptide with a sequence identical to one of the active sites of human Motoneuronotrophic Factor and is manufactured by solid phase synthesis. Preclinical research indicates it to be a neuro-protective agent in animal models of PD, other neuro-degenerative diseases and stroke. This trial is designed to test proof of principle, i.e. determine if a 2-week treatment with this agent can restore the non-functioning nigral dopaminergic neurons in PD over a 3 month period, during which the placebo-treated arm is expected to have little or no worsening of the total UPDRS (Unified Parkinson's Disease Rating Scale)score compared to baseline.

Study Objectives are:

1. To compare the safety and tolerability of GM608 with placebo in a population of patients with early PD.

2. To field test the study procedures for feasibility and efficiency

3. To determine if there is any hint that injections of GM608 might slow the rate of clinical worsening of PD.

Description:

Background The investigational drug GM608 is a synthetic oligopeptide containing 6 amino acids with a sequence identical to one of the active sites of human Motoneuronotrophic factor (MNTF), also referred to as GM6 in studies. MNTF is a novel human endogenous developmental stage neurotrophin for the nervous system with a specific human chromosome location.

The investigators' preclinical animal study has shown that intravenously injected GM608 is able to penetrate the blood-brain barrier and enter the brain. GM608 has shown neuroprotection in a variety of in vitro and animal models of numerous Central Nervous System (CNS) diseases including ischemic stroke, spinal cord injury, Parkinsons Disease (PD), amyotropic lateral sclerosis (ALS), multiple sclerosis (MS), Alzheimer's Disease (AD) and Huntington Disease (HD). In particular, the 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) and 6-hydroxydopamine (6-OHDA) mouse model for PD all showed GM608 has neuroprotective effect. GM608 also enhanced neuron cell survival very significantly in the cerebrospinal fluid (CSF) of patients with Huntington disease, MS, Stroke, Parkinson, Alzheimer and ALS.

This pilot trial is designed to test proof of principle, i.e. determine if a 2-week treatment with this agent can restore the nonfunctioning nigral dopaminergic neurons in PD over a 3month period, during which the placebo-treated arm is expected to have little or no worsening of the total UPDRS score compared to baseline. A Phase 1 Clinical Trial Study has been completed. The Phase 1 Trial primary objective is to determine the safety and tolerability and to establish the pharmacokinetic and pharmacodynamic properties of GM608 at 0.5, 1.5, and 5.0 mg/kg administered as a single bolus intravenous dose in human subjects and after 3 consecutive daily doses of GM608 at the highest safe and tolerated dose of 5.0 mg/kg. The Phase 1 study established that 3 consecutive daily doses of 5.0 mg/kg of GM602 are safe and tolerated.

Mechanism of Action Motoneuronotrophic factor (MNTF) is highly specific to the human nervous system. It is expressed rapidly during the first trimester of human fetal development, peaking at week nine. MNTF is a developmental stage regulatory (antisense) neuro-signaling molecule that binds perfectly on very specific receptors. Using In Silico Analysis, Genervon identified and developed as a drug candidate one of the active sites of MNTF, an analog of six amino acids named GM608.

In the investigators' testing for efficacy in Parkinson disease MPTP and 6-OHDA animal models, GM608 demonstrated a dose dependent attenuation of PD in the mice with 20 mg/kg showing the most efficacious. Behavioral, biochemical and histological analysis demonstrated the attenuation illustrating a unique effect for GM608 in PD. These data suggest that GM608 is effective in the mouse model of PD following IV injection and may be a potential treatment for PD patients.

In the investigators' in vitro study in Parkinson disease, treatment with wortmannin (PI3K inhibitor) abrogated the protective effects of GM608 on SH-SY5Y (a neuroblastoma cell line popular in studying neuroscience) cells which were subjected to salsolinol exposure for 24 hours. The results suggested that GM608 may function through the phosphatidylinositol 3-kinase (PI3K) pathway which is an important pathway in neuronal diseases.

Although the neuroprotective mechanism in each of the animal studies is not well understood, the investigators hypothesize that GM608 respond to specific distress signal anywhere from the human nervous system through a common underlying mechanism by triggering specific pathway(s), possibly through the PI3 pathway and other pathways that protect neural tissues by increasing or decreasing specific gene(s) expressions.

This is a single-center, prospective, randomized, double-blind, and placebo-controlled pilot study, involving 6 subjects not on any dopaminergic medication (i.e. levodopa or dopamine agonist). Subjects will be randomized 2:1 into one of two treatment arms: (1) 4 subjects will receive i.v. injections of GM608 and (2) 2 subjects will receive a matching placebo. Progression of clinical PD will be assessed using the UPDRS over 12 weeks. Safety and tolerability will also be compared between treated and placebo group.

There will be 2 weeks of active treatment, followed by 10 weeks of assessment without active treatment. During the 2-week active treatment phase, each subject will receive one IV bolus injection once a day for three times a week during these 2 weeks for a total of six injections. Subjects will be evaluated by UPDRS at screening, at baseline, and the ends of weeks 2 (at visit 6 after dosing), 6, and 12. The study duration for each subject is 12 weeks.

Recruitment information / eligibility

• Status: Completed
• Enrollment: 6
• Est. completion date: July 2014
• Est. primary completion date: July 2014
• Accepts healthy volunteers: No
• Gender: All
• Age group: 30 Years and older

Eligibility

Inclusion Criteria:

• with mild-moderate idiopathic PD diagnosed based on UK (United Kingdom) PD Brain Bank criteria.

• Age > 30

• Motor UPDRS Score = 15

• Hoehn & Yahr stage <3

• Diagnosis of PD <10 years

• Have fully completed informed consent form

• May be on antiparkinsonian medications of an MAO-B (monoamine oxidase -B) inhibitor, an anticholinergic, or amantadine, but not levodopa or dopamine agonist

Exclusion Criteria:

• Patients with atypical parkinsonism: such as suspected progressive supranuclear palsy (PSP), multiple system atrophy (MSA) or Corticobasal degeneration (CBD) and secondary parkinsonism such as normal-pressure hydrocephalus (NPH), drug-induced, or vascular parkinsonism.

• Patients with uncertainty as to having classical Parkinson disease, such as those who might have scans without evidence of dopaminergic deficit (SWEDDs)

• Patients not willing to give an informed consent

• Patients who are on a dopaminergic medication (levodopa or dopamine agonist)

• Presence of a medical or psychiatric comorbidity that can compromise participation in the study

Related Conditions & MeSH terms

• Parkinson Disease
• Parkinson's Disease

Intervention

Drug:
• GM608
For GM608: 320 mg/dose reconstituted with 6.4 mL bacteriostatic saline. Administer 6.4 mL GM608 dosing solution by intravenous (IV) bolus over 1 min, on Monday, Wednesday, Friday for two consecutive weeks.
• Placebo Comparator
For Placebo: Administer 6.4 mL Bacteriostatic saline by intravenous (IV) bolus over 1 min, on Monday, Wednesday, Friday for two consecutive weeks.

Locations

Country	Name	City	State
United States	Columbia University Medical Center/NY Presbyterian Hospital	New York	New York

Sponsors (2)

Lead Sponsor	Collaborator
Genervon Biopharmaceuticals, LLC	Columbia University

Country where clinical trial is conducted

United States, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Other	Secondary analyses will consider a comparison of slopes using a mixed-model approach with treatment as a fixed effect and subject-specific slopes as a random effect.	Measure the slopes of UPDRS change	12 weeks
Primary	The change from the mean total UPDRS score of the combined screening and baseline visits to the total UPDRS score at the Week-12 visit, comparing treated with placebo.Compare safety and tolerability with placebo.	Measure UPDRS and the change from the mean total UPDRS score of the combined screening and baseline visits to the total UPDRS score at the Week-12 visit, comparing treated with placebo.Compare safety and tolerability with placebo.	Baseline, week 2, week 6, week 12
Secondary	Change in total UPDRS between the mean screening-baseline visits and end of Week 2 (at visit 6 after dosing), and week 6, comparing the two arms of the study encompassing the entire cohort of 6 subjects.	Measure UPDRS and the Change in total UPDRS between the mean screening-baseline visits and end of Week 2 (at visit 6 after dosing), and week 6, comparing the two arms of the study encompassing the entire cohort of 6 subjects.	Baseline, week 2, week 6
Secondary	Change in UPDRS sub-scores (Mental, Activities of Daily Living, Motor) between the mean screening-baseline visits and ends of Week 2 (at visit 6 after dosing), 6, and 12, comparing the two arms of the study encompassing the entire cohort of 6 subjects.	Measure UPDRS subscores and the Change in UPDRS sub-scores (Mental, Activities of Daily Living, Motor) between the mean screening-baseline visits and ends of Week 2 (at visit 6 after dosing), 6, and 12, comparing the two arms of the study encompassing the entire cohort of 6 subjects.	Baseline, week 2, week 6, week 12
Secondary	Time to the development of sufficient disability to require a change in symptomatic therapy.	Measure the Time to the development of sufficient disability to require a change in symptomatic therapy.	12 weeks
Secondary	Proportion of subjects requiring additional symptomatic treatment due to disability.	Measure the proportion of subjects requiring additional symptomatic treatment due to disability.	12 weeks
Secondary	Change in Schwab & England ADL (activity of daily living) score from baseline to Week 2 (at visit 6 after dosing), 6, or 12.	Measure Schwab & England ADL score and its change from baseline to Week 2 (at visit 6 after dosing),	Baseline, week 2, week 6, week 12
Secondary	Change in Hoehn & Yahr score (H&Y), Beck Depression Inventory (BDI), and Montreal Cognitive Assessment (MOCA) scores from baseline to Week 2 (at visit 6 after dosing), 6, or 12.	Measure Hoehn & Yahr score (H&Y), Beck Depression Inventory (BDI) and MontrealCognitive Assessment (MOCA) scores and their changes from baseline to Week 2, Week 6 and Week 12	Baseline, week 2, week 6, week 12