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| Name | Class |
|---|---|
| Columbia University | OTHER |
| Massachusetts General Hospital | OTHER |
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GM604 is an endogenous human embryonic stage neural regulatory and signaling peptide that controls the development, monitoring and correction of the human nervous system. Neurological diseases are multisystem, multifactorial, and single target drugs are ineffective. Genervon's Master Regulators play a significant role in embryonic/fetal nervous system development and are potent disease modification drug candidates modulating many pathways including inflammation, apoptotic, and hypoxia. The study drug is an regulatory peptide with a sequence identical to one of the active sites of human Motoneuronotrophic Factor and is manufactured by solid phase synthesis. Pre-clinical research indicates it to be a neuro-protective agent in animal models of ALS, motorneuron diseases, PD, other neuro-degenerative diseases and stroke. GM604 controls and modulates over many known and significant ALS genes with positive effects interactively and dynamically through multiple pathways, and up to twenty-two biological processes, including neuro-protection, neurogenesis, neural development, neuronal signaling, neural transport, and other processes. GM6 is not a cocktail of drugs, but one master regulator peptide drug that functions through multiple pathways. Genervon hypothesized that studying the biomarkers of protein expressions of these ALS genes such as superoxide dismutase 1 (SOD1) and the protein expression of substances such as tau, neurofilament - heavy (NF-H), Cystatin C which were indications of degeneration of neuron in the CSF collected from ALS patients will provide information of the possible GM604's mechanisms of action in treating ALS. 1. This pilot trial is designed to test proof of principle, i.e. determine if a 2-week IV bolus treatment with this agent can (1) change ALS protein expression (target biomarkers and efficacy biomarkers) after treatment (2) have preliminary effects measures of ALS disease clinical progression.
Study Objectives are:
Background
The conclusion is that GM604 was found to be efficacious in an in vivo mouse model of neurological disease. The effectiveness of GM604 was dose-dependent and indicates that GM604 may be beneficial in treating various neurological disorders.
Rationales
IND 77,789: "A Phase 2 double blinded, randomized, placebo controlled dose escalation Study to Evaluate the Efficacy and the Safety of GM602 in Patients with Acute Middle Cerebral Artery Ischemic Stroke within an 18 h-hour treatment window. Acronym/Title is GMAIS. GM602 received fast track designation for ischemic stroke in 2007. The stroke trial has not completed enrollment and has not unblinded the treatment randomization to generate drug related safety report.
IND 109,441: "GM602 in A Phase IIA Pilot double-blinded, randomized, placebo controlled trial in mild to moderate Parkinson Disease (PD). Acronym/Title is GAP-PD. The PD trial is recruiting patients.
Possible GM604 Mechanisms of Action (MOA) in ALS
Use of Biomarkers for ALS
Most late-phase clinical trials across all diseases fail to demonstrate drug efficacy between case and controls. The incorporation of biomarkers within clinical trials may reduce this 'drug attrition' rate. The biomarkers to be incorporated into clinical trials can be subdivided into:
Genervon hypothesized that modulating disease causing genes may modulate ALS disease progression.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| GM604 treated | Experimental | 8 subjects will receive GM604. Each GM604 treated subject will receive a slow IV bolus injection (~1min) of 6.4 mL (320mg @50 mg/mL=6.4 mL) for each dose. A total of 6 doses will be administered over two weeks (on Mondays, Wednesdays and Fridays for the first 2 weeks). |
|
| Placebo comparator | Placebo Comparator | 4 subjects will receive placebo. 6.4 mL Bacteriostatic saline will be used for the Placebo group. Injections will be given to the subject in the same manner as in GM604 treated group. A total of 6 doses will be administered over two weeks (on Mondays, Wednesdays and Fridays for the first 2 weeks). |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| GM604 | Drug | GM604 treated group subject will receive a slow IV bolus injection (~1min) of 6.4 mL (320mg @50 mg/mL=6.4 mL) for each dose. A total of 6 doses will be administered over two weeks (on Mondays, Wednesdays and Fridays for the first 2 weeks). |
| Measure | Description | Time Frame |
|---|---|---|
| Efficacy by percent change in biomarker in th CSF at week 12 from baseline | Efficacy by percent change in biomarker in the CSF at week 12 from baseline: (a) Efficacy biomarkers (b) Target biomarkers (c) Efficacy/target biomarkers | baseline, week 2, week 12 |
| Safety by measuring 1. adverse event frequency and severity, changes in vital signs, clinical laboratory values. 2. Serious adverse event frequency | Safety: 1. adverse event frequency and severity, changes in vital signs, clinical laboratory values. 2. Serious adverse event frequency | baseline, week 2, week 12 |
| Tolerability by measuring the ability to complete the first 2 weeks of active treatment in the study | Tolerability: The ability to complete the first 2 weeks of active treatment in the study | Baseline, week 2, week 12 |
| Measure | Description | Time Frame |
|---|---|---|
| ALSFRS-R (Amyotrophic Laeral Sclerosis Functional Rating Scale - Revised) | Progressive change in ALSFRS-R of each patient determined from the following data points:1) symptom onset, 2) baseline, 3) end of week 2 examination, 4) end of week 6 examination and 5) end of week 12 examination. | Symptom onset, screening, baseline, week 2, week 6, week 12 |
| Measure | Description | Time Frame |
|---|---|---|
| comparison of slopes (change in the rate of decline)of disease progression | Secondary analyses may consider a comparison of slopes (change in the rate of decline) for any hint of disease modification using placebo outcomes in patients matched for baseline features from a large database of recent clinical trials by NEALS showing stable rates of decline as historical controls. | Symptom onset, baseline, week 2, week 6, week 12 |
Inclusion Criteria:
Exclusion Criteria:
History of liver disease, severe renal failure, diabetes, coronary heart disease, cancer
Clinically significant EKG abnormality at screening
Any comorbid condition which would make completion of the trial unlikely
FVC < 65%
Presence of a bleeding disorder
Allergy to local anesthetics
Problem with CSF pressure
Topical or other skin infection at the lumbar puncture site
BMI > 32 kg/m2
Medical or surgical conditions in which a lumbar puncture is contraindicated
Use of any anti-platelet or anticoagulant drugs, such as plavix, aggrenox, ticlid, warfarin or coumadin
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| Name | Affiliation | Role |
|---|---|---|
| Hiroshi Mitsumoto, MD | Columbia Medical Center NY | Principal Investigator |
| Merit Cudkowicz, MD | Massachusetts General Hospital | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Massachusetts General Hospital | Boston | Massachusetts | 02114 | United States | ||
| Columbia Medical Center NY |
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| ID | Term |
|---|---|
| D000690 | Amyotrophic Lateral Sclerosis |
| D002493 | Central Nervous System Diseases |
| D009410 | Nerve Degeneration |
| D035583 | Rare Diseases |
| D028361 | Mitochondrial Diseases |
| ID | Term |
|---|---|
| D013118 | Spinal Cord Diseases |
| D009422 | Nervous System Diseases |
| D016472 | Motor Neuron Disease |
| D019636 | Neurodegenerative Diseases |
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| Placebo comparator | Drug | Placebo comparator group subject will receive a slow IV bolus injection (~1min) of 6.4 mL bacteriostatic saline for each dose. A total of 6 doses will be administered over two weeks (on Mondays, Wednesdays and Fridays for the first 2 weeks). |
|
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| Forced Vital Capacity (FVC) | Progressive change in Forced Vital Capacity (FVC) from the following data points: 1) symptom onset, 2) baseline, 3) end of week 2 examination, 4) end of week 6 examination and 5) end of week 12 examination. | Symptom onset, baseline, week 2, week 6, week 12 |
| Time Up and Go (TUG) | Progressive change in Forced Vital Capacity (FVC) from the following data points: 1) symptom onset, 2) baseline, 3) end of week 2 examination, 4) end of week 6 examination and 5) end of week 12 examination. | Symptom onset, baseline, week 2, week 6, week 12 |
| muscle strength | Progressive muscle strength change measured by HHD (handheld dynamometry testing score) from the following data points: 1) symptom onset, 2) baseline, 3) end of week 2 examination, 4) end of week 6 examination and 5) end of week 12 examination. | Symptom onset, baseline, week 2, week 6, week 12 |
| Biomarker in blood | Percentage changes in Biomarkers in blood between baseline and 1) the end of week 1, 2) end of week 2, 3) end of week 6 and 4) end of week 12. Comparing the changes encompassing the entire cohort of 10 subjects. | baseline, week 2, week 6, week 12 |
| Mortality rate | Report all death as mortality rate | baseline, week 2, week 6, week 12 |
| stratification of patients by symptoms | Secondary analysis to allow a-priori stratification of patients by their symptoms if available
| Symptom onset, baseline, week 2, week 6, week 12 |
| New York |
| New York |
| 10032 |
| United States |
| D057177 | TDP-43 Proteinopathies |
| D009468 | Neuromuscular Diseases |
| D057165 | Proteostasis Deficiencies |
| D008659 | Metabolic Diseases |
| D009750 | Nutritional and Metabolic Diseases |
| D010335 | Pathologic Processes |
| D013568 | Pathological Conditions, Signs and Symptoms |
| D020969 | Disease Attributes |