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TOKYO, Jan. 2 -- Tremors and other symptoms associated with Parkinson's
disease can be reduced significantly by the antiepileptic drug Zonegran
(zonisamide) without an increase in dyskinesias, according to Japanese
researchers.


Patients with Parkinson's disease resistant to levodopa who received Zonegran
in two of three different doses had significant improvements in Parkinson's
disease rating-scale scores compared with patients who received placebo,
found Miho Murata, M.D., Ph.D., of the National Center of Neurology and
Psychiatry here and colleagues.
"Zonisamide treatment improved all main Parkinson disease symptoms in these
patients, including tremor and other disabling dyskinesias," wrote Dr. Murata
and colleagues in the Jan. 2 issue of Neurology. "This is consistent with
findings from other, smaller studies."
The investigators previously published a case report and results of a small
open-label study indicating that Zonegran could improve the main symptoms of
Parkinson's disease, including limb rigidity, tremor, postural instability,
and motor fluctuations that occur during wearing-off from levodopa.
In the current multicenter study, 347 patients with Parkinson's disease who
were not well controlled on levodopa were randomly assigned, after a two-week
placebo-controlled washout phase, to either Zonegran in doses of 25, 50, or
100 mg daily, or placebo, as an adjunct to levodopa. Patients were treated
for 12 weeks, followed by a two-week dose-reduction phase.
The primary efficacy endpoint was change from baseline in the total score of
the Unified Parkinson's Disease Rating Scale (UPDRS) Part III at the final
assessment point.
Secondary endpoints included change from baseline in total daily "off" time.
total scores of UPDRS Parts I, II, and IV, and Modified Hoehn and Yahr Scale
scores.
The investigators also looked at the safety of the therapy based on the
incidence of adverse events.
They found that among the 279 patients who completed the study, there were
significant improvements in the primary endpoint in both the 25-mg and 50-mg
groups compared with placebo.
The changes in the UPDRS Part III total score from baseline at final
assessment were -2.0 + 0.8 (standard error of the mean) in the placebo group,
-6.3 + 0.8 in the 25 mg group, -5.8 + 0.8 in the 50-mg group, and -4.6 + 0.8
in the 100-mg group. The improvement over placebo was significant for both
the 25-mg group (P=0.001, Dunnett test) and 50-mg group (P=0.003).
The proportion of responders -- patients with a 30% or greater reduction in
UPDRS Part III total score from baseline at final assessment -- was 22% in
the placebo group, and 35.1%, 38.8% and 31.7% in the 25, 50 and 100 mg
groups, respectively. The difference versus. placebo group was significant
for the 50-mg dose.
"The duration of 'off' time was significantly reduced in the 50-mg and 100-mg
groups versus placebo," the investigators wrote. "Dyskinesia was not
increased in zonisamide groups."
Adverse events that occurred more frequently among patients on Zonegran
included somnolence, apathy, weight loss, and constipation. The incidence of
adverse events was similar between the 25-mg, 50-mg, and placebo groups, but
higher in the 100-mg group.
Although patients on Zonegran appeared to benefit from the drug, it's unclear
why, the authors noted.
"Zonisamide has no affinity to dopamine receptors (D1-D5) or dopamine
transporter," they wrote. "Zonisamide also has no direct effects on glutamate
receptors, adenosine receptors, or serotonin receptors, which have been
suggested as possible sites of action for anti-PD drugs, other than the
dopaminergic system."
Although they had previously hypothesized that activation of dopamine
synthesis and moderate inhibition of monoamine oxidase type B were the
primary mechanisms mediating the effects of Zonegran in Parksison's, there
were no differences in the efficacy of the antiepileptic when it was
administered either with or without a monoamine oxidase type B-inhibitor.
The study was supported by Dainippon Sumitomo Pharma, developer of Zonegran.
Authors' financial disclosures, if any, were not specified.
Additional Parkinson's Disease Coverage


Primary source: Neurology
 Source reference:
Murata M et al. "Zonisamide improves motor function in Parkinson disease A
randomized, double-blind study." Neurology 2007;68:45-50

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