Safety and Preliminary Effectiveness of AV650 in Patients With Spasticity Associated With Multiple Sclerosis
NCT ID: NCT00532532
Last Updated: 2008-11-04
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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TERMINATED
PHASE2
150 participants
INTERVENTIONAL
2007-09-30
2008-11-30
Brief Summary
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1. To determine whether AV650 is safe for patients with multiple sclerosis;
2. To gather some early evidence as to whether AV650 is effective in treating spasticity in patients with multiple sclerosis; and,
3. To assess what the body does with AV650 once it is ingested (Germany and Czech Republic sites only).
Detailed Description
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Conditions
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Keywords
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
QUADRUPLE
Study Groups
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1
AV650 low dose
tolperisone HCl
Low dose AV650 three times a day orally for 5 weeks; followed by optional continuation on either low dose or high dose AV650, as tolerated, for 24 weeks
2
AV650 high dose
tolperisone HCl
High dose AV650 three times a day orally for 5 weeks; followed by optional continuation on either low dose or high dose AV650, as tolerated, for 24 weeks
3
Placebo
tolperisone HCl
Placebo three times a day orally for 5 weeks; followed by optional continuation on either low dose or high dose AV650, as tolerated, for 24 weeks
Interventions
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tolperisone HCl
Low dose AV650 three times a day orally for 5 weeks; followed by optional continuation on either low dose or high dose AV650, as tolerated, for 24 weeks
tolperisone HCl
High dose AV650 three times a day orally for 5 weeks; followed by optional continuation on either low dose or high dose AV650, as tolerated, for 24 weeks
tolperisone HCl
Placebo three times a day orally for 5 weeks; followed by optional continuation on either low dose or high dose AV650, as tolerated, for 24 weeks
Eligibility Criteria
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Inclusion Criteria
* Signed and dated informed consent
* Definite MS as per Poser or MacDonald Criteria (either relapsing remitting or secondary progressive course)
* Expanded Disability Status Score (EDSS) from 3.0 to 6.5 (inclusive) at Screening
* Stable MS for at least 30 days before screening
* Female of child bearing potential and male subjects whose partner is of child bearing potential who are willing to ensure that they or their partner use effective double-barrier contraception during the study and for 90 days thereafter
* If female, be neither pregnant nor nursing (Confirmation that the subject is not pregnant must be established by a negative serum hCG pregnancy test at baseline.)
* Significant spasticity in at least two muscle groups defined as a score of 2 or more on the Ashworth scale for each muscle group
* If a subject is on anti-spastic treatments, the dosage, frequency, and route of administration must be stable for at least 30 days before Screening
* If a subject is on MS treatments, the dosage, frequency, and route of administration must be stable for at least 30 days before Screening
Exclusion Criteria
* Significant changes in anti-spasticity medications (dosage, frequency, or route of administration) within 30 days of Screening
* Known hypersensitivity to tolperisone HCl, its components, or other lidocaine/lidocaine-like products
* Use of tolperisone HCl within 30 days of screening
* Significant changes in MS treatments (dosage, frequency, or route of administration) within 30 days of Screening
* Spasticity due to neurological disorders other than MS
* Any psychiatric disorder or cognitive impairment that precludes fully informed consent or safe participation in the study
* Subjects who have suffered an acute relapse of MS or who continue to suffer from an acute relapse of MS within 90 days of Baseline
* History of alcohol or substance abuse within one year of Screening
* Concurrent clinically significant immunologic, pulmonary, renal, hepatic, or endocrine disease and/or other unstable or major disease other than MS
* Clinically significant cardiovascular disorders, such as ischemic heart disease, arrhythmias, poorly controlled hypertension, or acute myocardial infarction
* QT prolongation greater than 480 msec or greater than 450 msec if accompanied by a partial bundle branch block, or other ECG abnormality in the judgment of the Investigator
* Diastolic blood pressure \<50mmHg or \>105mmHg; heart rate \<50 beats per minute (bpm) or \>110bpm, after 3 minutes in a sitting position; heart rate by ECG \<50bpm or \>110bpm
* History of epilepsy (except childhood febrile seizures)
* Current malignancy or history of malignancy that has not been in remission for more than five years, except basal cell skin carcinoma and cervical cancer (with treatment)
* Female subject who is pregnant, nursing, or planning pregnancy during the course of the study
* Scheduled elective surgery or other procedures requiring general anesthesia during the study
* Subject who is terminally ill in the judgment of the Investigator
* Subject who is inappropriate for placebo medication in the judgment of the Investigator
* Systemic corticosteroid therapy within 28 days of randomization, with the exception of inhaled medications for asthma
* Exacerbation of MS within 30 days of Baseline
* Regular levo-dopa therapy within 7 days of randomization
* Subjects taking antiarrhythmic medications
* Donation of blood during the study
18 Years
70 Years
ALL
No
Sponsors
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Avigen
INDUSTRY
Responsible Party
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Avigen, Inc.
Principal Investigators
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Glenn Morrison, MSc, PhD
Role: STUDY_DIRECTOR
Avigen, Inc.
Locations
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Annes University Hospital
Brno, , Czechia
University Hospital Hradec Kralove
Hradec Králové, , Czechia
University Hospital Plzen
Pilsen, , Czechia
University Hospital Motol
Prague, , Czechia
Facharzt fur Neurologie
Bad Saarow, , Germany
Facharztin fur Neurologie und Psychiatrie
Berlin, , Germany
Facharzt fur Neurologie und Psychiatrie
Berlin, , Germany
Private practice
Berlin, , Germany
Neurological practice
Bochum, , Germany
Neurological practice
Cologne, , Germany
Neuro-Consil GmbH
Düsseldorf, , Germany
X-pert-med GmbH
Gräfelfing, , Germany
Asklepios Klinik Nord-Heidberg
Hamburg, , Germany
City Hospital #33
Nizhny Novgorod, , Russia
Regional Clinical Hospital named Semashko
Nizhny Novgorod, , Russia
Institute of Human Brain
Saint Petersburg, , Russia
Leningrad Regional Clinical Hospital
Saint Petersburg, , Russia
Nikolaevskaya Hospital, Complex Rehabilitation Department
Saint Petersburg, , Russia
Clinical Center of Serbia Institute of Neurology
Belgrade, , Serbia
Clinical Center Nis Clinic of Neurology
Niš, , Serbia
Ivano-Frankivsk Regional Clinical Hospital
Ivano-Frankivsk, , Ukraine
Central Clinical Hospital Ukrzalinznytsi (Dept. Neur. No. 1)
Kharkiv, , Ukraine
Central Clinical Hospital Ukrzalinznytsi (Dept. Neur. No. 3)
Kharkiv, , Ukraine
Institute of Neurology, Psychiatry and Narcology of AMS of Ukraine
Kharkiv, , Ukraine
Institute of Clinical Radiology of the Scientific Centre of Radiation Medicine of the AMS of Ukraine
Kyiv, , Ukraine
Odesa Regional Psychoneurological Dispensary
Odesa, , Ukraine
M.O.Semashko Republican Clinical Hospital
Simferopol, , Ukraine
Uzhgorod Regional Centre of Neurosurgery and Neurology
Uzhhorod, , Ukraine
Countries
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Other Identifiers
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AV650-018
Identifier Type: -
Identifier Source: org_study_id