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Increased neostriatal dopamine activity after intraperitoneal or
intranasal administration of L-DOPA: on the role of benserazide
pretreatment: rat study
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L-DOPA provides the most potent medication to treat Parkinson's disease,
and such systemic treatment is usually combined with a peripheral amino
acid decarboxylase inhibitor to amplify its central effectiveness.

Since L-DOPA can lose its efficacy or can lead to adverse effects with
prolonged application, current pharmacokinetic and dynamic research is
aimed at improving the drug's applicability.

In a previous study, performed with in vivo microdialysis in the
anesthetized rat, we have shown that intranasal L-DOPA administration
(without prior decarboxylase inhibition) can increase extracellular
dopamine levels in the neostriatum.

Using similar experimental conditions in the present experiment, we tested
the neurochemical effects of L-DOPA treatment in combination with the
peripheral amino acid decarboxylase inhibitor benserazide.

In accordance with other data, it was found that the combination of i.p.
benserazide and i.p. L- DOPA led to pronounced increases of extracellular
levels of dopamine, dihydroxyplenylacetic acid and homovanillic acid in the
neostriatum, whereas i.p. L-DOPA alone only moderately increased dopamine,
but strongly increased the metabolite levels.

Furthermore, increased dopamine levels, and weaker increases of
dihydroxyplenylacetic acid and homovanillic acid were observed after i.p.
benserazide followed by intranasal L-DOPA.

Finally, we found that i.p. benserazide alone can lead to pronounced
increases in neostriatal dopamine and moderate increases of
dihydroxyplenylacetic acid levels, whereas it did not affect homovanillic
acid.

Thus, not only the combination of L-DOPA (i.p. or intranasal) with the
presumed peripheral L-DOPA decarboxylase inhibitor benserazide, but also
each component alone can affect dopamine activity in the brain.

Especially the findings with benserazide treatment might be of relevance
for understanding the mechanisms of current L-DOPA therapy, since they
indicate that part of the treatment's actions may possibly be determined by
central dopaminergic effects of the accompanying amino acid decarboxylase
inhibitor.


Synapse 1997 Dec;27(4):294-302
Silva MA, Mattern C, Hacker R, Tomaz C, Huston JP, Schwarting RK
Heinrich-Heine-University of Dusseldorf, Germany.
PMID: 9372552    UI: 98039821
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