Multiple System Atrophy Clinical Trial
Official title:
Evaluate the Long-term (3 Months) Efficacy of L-threo DOPS (DroxiDopa) on Orthostatic Hypotension Symptoms and Other Non-motor Symptoms in Patients With Multiple System Atrophy (MSA). Comparative Study Versus Placebo
Evaluate the effects of L-Threo DOPS on orthostatic hypotension symptoms and other non-motor symptoms in patients with Multiple System Atrophy (MSA) after 12 weeks following randomization to continued therapy with droxidopa or placebo.
Background :
Multiple system atrophy (MSA) is a rare, sporadic progressive neurodegenerative disorder,
rapidly leading to severe disability and impairment of quality of life. MSA is characterized
by a variable combination of a poor levodopa parkinsonism and /or cerebellar ataxia and
autonomic failure (cardiovascular and / or bladder and sexual dysfunction) (Gilman et al,
2008). The prevalence is approximately 4-5 cases per 100 000 inhabitants.
Orthostatic hypotension (OH) is one of the major symptoms of MSA, present in a large majority
of patients, leading to significant disability because of impaired balance, falls and
possibly syncope. Drugs available to treat OH in this disease are very limited.
L-ThreoDOPS (L DOPS or DroxiDopa) is an orally administered synthetic catecholamine acid that
is converted to the sympathetic neurotransmitter norepinephrine (NE) through a single step of
decarboxylation by the endogenous enzyme 3,4-dihydroxyphenylalanine (DOPA) decarboxylase. It
prevents symptoms related to OH by central and/peripheral mechanisms. This drug is currently
developed for "neurogenic OH" by Chelsea Therapeutics on the basis of short duration
placebo-controlled randomized trials. Besides an expected effect on OH, L-DOPS may also, by
noradrenergic stimulation, improve some motor and non-motor symptoms common and disabling in
MSA patients such as akinesia and fatigue.
In this context, the French reference center for MSA and the 12 national centers with
identified skills to manage this disease, propose to conduct a national multicenter
randomized clinical trial versus placebo to evaluate the long term efficacy (3 months) of
L-threo DOPS on the OH and other non-motor symptoms in MSA patients.
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