LISTSERV 16.0 - PARKINSN Archives

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Somatic delivery of catecholamines in the striatum attenuate parkinsonian
symptoms and widen the therapeutic window of oral sinemet in rats.
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Guidelines for clinical transplantation studies for Parkinson's disease
emphasize that transplants should be considered as an adjunct to systemic
L-DOPA, yet few preclinical studies have specifically assessed the
potential of transplants as an adjunct to the clinical gold standard
treatment.

The objectives of the present study were to determine if encapsulated PC12
cells implanted in rats with severe unilateral dopamine depletions:

(i) have a direct therapeutic effect on measures of parkinsonian symptoms;
and/or
(ii) increase the therapeutic window of oral sinemet in this model.

Rats with severe unilateral dopamine depletions received striatal implants
of encapsulated PC12 cells producing dopamine and L-DOPA.

These rats were tested on a battery of behavioral measures of parkinsonian
symptoms, at a range of doses of oral sinemet (0, 12, 24, and 36 mg/kg).

Stereotypies/dyskinesias were also quantified after high doses of oral
sinemet (36 and 50 mg/kg).

The results confirm that parkinsonian symptoms can be quantified in rats
with severe dopamine depletions, and the validity and clinical relevance of
these measures are supported by the fact that the clinical gold standard
treatment, oral sinemet, attenuates these parkinsonian symptoms.

Somatic delivery of dopamine and L-DOPA, directly to the dopamine-depleted
striatum, also attenuates parkinsonian symptoms.

In fact, the magnitude of the therapeutic effect produced by continuous,
site-specific, somatic delivery of dopamine and L-DOPA was larger than the
effect produced by acute, systemic, oral sinemet.

The beneficial effects of oral sinemet and striatal implants of
catecholamine-producing devices were additive, but there were no adverse
effects related to striatal catecholamine-producing devices, and these
devices did not increase the adverse effects related to oral sinemet.

Therefore, striatal implants of catecholamine-producing devices have direct
therapeutic effects which are fairly robust, and they widen the therapeutic
window of oral sinemet.


Exp Neurol 1997 May;145(1):130-140
Lindner MD, Plone MA, Mullins TD, Winn SR, Chandonait SE, Stott JA,
Blaney TJ, Sherman SS, Emerich DF
Cyto Therapeutics Inc., Providence, Rhode Island 02906, USA.
PMID: 9184116, MUID: 97327449
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