Parkinson's Disease Clinical Trial
Official title:
Mucuna Pruriens Therapy in Parkinson's Disease: a Double-blind, Placebo-controlled, Randomized, Crossover Study.
In low-income areas worldwide, most patients with Parkinson's disease (PD) cannot afford
long-term Levodopa therapy. A potential therapeutic option for them is the use of a legume
called Mucuna Pruriens var. Utilis (MP), which has seeds with a high levodopa content (5-6%)
and grows in all tropical areas of the world. MP powder is very cheap (total annual cost for
a PD patient: 10-15 US $). The aim of this study is to assess efficacy and tolerability of
acute and chronic use of MP compared to standard Levodopa therapy.
The primary objective of this study is to investigate efficacy of acute levodopa challenge
using MP in comparison to levodopa with a Dopa Decarboxylase Inhibitor (LD+DDCI) and without
(LD-DDCI) and placebo.
The secondary objectives are to investigate safety of acute intake of MP as well as efficacy
and safety of chronic intake of MP over a 8-week period in comparison to usual LD+DDCI home
therapy.
Background: Levodopa is the gold standard in the treatment of Parkinson's disease (PD).
However, in low-income areas worldwide, most patients with PD cannot afford chronic therapy
with levodopa. It is therefore mandatory to identify an interventional strategy designed to
ease the economic burden of pharmacological management of PD in developing countries. A
potential therapeutic option for them is the use of a legume called Mucuna Pruriens variant
Utilis (MP), which has seeds containing high LD concentrations and grows spontaneously in
all tropical and subtropical areas of the world, including South America, Africa and Asia.
It is considered an invasive plant, as it grows rapidly without any particular measure
needed to ensure its growth. The cost of home preparation of MP roasted powder is negligible
and it is easy to store for a long time. LD was isolated from MP seeds for the first time in
1937 and its concentration therein was estimated to be 4-6%. MP is also known as Ayurvedic
remedy for PD since ancient times.
Preliminary data: Published studies in parkinsonian rats, primates and humans suggest that
MP may be used to improve PD motor symptoms without major side effects.
In a preliminary study, we analyzed 25 samples of MP from Africa, Latin America and Asia and
measured the content in LD and anti-nutrients. We found that LD concentration in roasted
powder samples was consistent with previous literature (median[Inter-Quartile Range]
5.3%[5.17-5.5]) and found no harmful anti-nutrients in all MP samples.
Study population: patients with diagnosis of idiopathic PD, including sustained response to
levodopa and presence of motor fluctuations defined as predictable wearing-off,
unpredictable ON-OFF fluctuations and sudden OFF periods.
Setting: Clinica Niño Jesus, Santa Cruz (Bolivia). This setting is chosen because the local
neurologist Dr. Janeth Laguna has long-term experience on MP therapy in patients with PD
(approximately 10 years). She started using MP because patients living in rural areas asked
her to use this cheap source of LD to reduce the monthly cost of anti-PD therapy. In her
experience, J.L. never recorded any serious adverse event (personal communication).
Preliminary Laboratory Test: The levodopa content in the powder obtained from roasted seeds
of Bolivian black ecotype of MP was tested in a laboratory in Milan (Italy) and found to be
5.7%. No alkaloids or major antinutrients were found.
Objectives:
The primary objective is to assess the efficacy of acute challenge of MP roasted powder
compared to Levodopa formulations with a dopa-decarboxylase inhibitor (LD-DDCI) and without
(LD+DDCI), and placebo. Levodopa dose with DDCI is administered at 3.5 mg/kg, while Levodopa
without DDCI is administered at the equivalent dose. This conversion factor is 5-fold, based
on published studies comparing clinical and pharmacokinetic Levodopa effects with and
without a DDCI and a previous double blind study on MP in patients with PD. For example,
100mg of Levodopa plus DDCI (either Benserazide or Carbidopa) corresponds to 500mg of
Levodopa without any DDCI, obtained by administration of 8.75 grams of MP roasted powder
(considering 5.7% of Levodopa in the bolivian ecotype of MP). Levodopa dose from MP is
planned to be administered at not only at the equivalent dose of LD+DDCI (i.e. 5-fold), but
also at the lower dosage of 3.5-fold.
Design: double-blind, randomized, placebo controlled, crossover study of acute response to
levodopa-based therapies Duration: 3-6 hours for each treatment arm.
The secondary objectives include additional measures of efficacy of acute intake of MP as
well as efficacy and safety of chronic use of MP as the only source of levodopa compared to
optimized home LD+DDCI therapy. This latter part is performed after completion of the acute
challenge part of the study.
Design: single-blind, randomized, crossover study of chronic response to levodopa-based
therapies.
Duration: 8 weeks per treatment arm plus 3-week dose adjustment period. Initial
levodopa-based therapy regimen (either MP therapy or Levodopa/Benserazide) may be adjusted
for a period up to 3 weeks to optimize daily motor status during waking hours. After this
period, patients enter the study and levodopa daily dose must be left unchanged throughout
the 16-week course of the study.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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