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Effects of systemic carbidopa on dopamine synthesis in rat hypothalamus and striatumSignificant concentrations of carbidopa (CD) were found in rat hypothalamus, striatum, and in striatal microdialysis efflux after intraperitoneal administration of the drug. Efflux levels peaked one hour after administration of 100 mg/kg at 0.37 microg/kg or about 2 percent of serum levels. Concurrent CD levels in hypothalamus and striatum were about 2.5 percent and 1.5 percent, respectively, of corresponding serum levels. Levels of dopamine and its principal metabolites in striatal efflux were unaffected. The removal of the brain blood by saline perfusion decreased the striatal and hypothalamic CD concentrations only by 33 percent and 16 percent, respectively. In other rats receiving both CD and levodopa (LD), brain L-dopa, dopamine, and 3,4-dihydroxyphenvlacetic acid (DOPAC) levels after one hour tended to be proportionate to LD dose. When the LD dose remained constant, increasing the CD dose dose-dependently enhanced L-dopa levels in the hypothalamus and striatum. However, dopamine levels did not increase but, in contrast, decreased dose-dependently (although significantly only in the hypothalamus). CD also caused dose-dependent decrease in striatal 3-O-methyldopa (3-OMD) and in striatal and hypothalamic homovanillic acid (HVA), when the LD dose was 50 mg/kg. We conclude that, at doses exceedimg 50 mg/kg, sufficient quantities of CD enter the brain to inhibit dopamine formation, especially in the hypothalamus. Moreover, high doses of LD/CD, both of which are themselves catechols, can inhibit the O-methylation of brain catecholamines formed from the LD.
Document ID
19930074681
Acquisition Source
Legacy CDMS
Document Type
Reprint (Version printed in journal)
Authors
Kaakkola, S.
(Helsinki Univ. Finland)
Tuomainen, P.
(Helsinki Univ. Finland)
Wurtman, R. J.
(Massachusetts Inst. of Tech. Cambridge, MA, United States)
Maennistoe, P. T.
(Helsinki Univ. Finland)
Date Acquired
August 16, 2013
Publication Date
September 20, 1991
Subject Category
Aerospace Medicine
Report/Patent Number
REPT-811
NAS 1.26:192856
NASA-CR-192856
Accession Number
93N72128
Funding Number(s)
CONTRACT_GRANT: NAG2-210
Distribution Limits
Public
Copyright
Public Use Permitted.
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