Literature DB >> 1867835

Central action of benserazide after COMT inhibition demonstrated in vivo by PET.

J Tedroff1, P Hartvig, P Bjurling, Y Andersson, G Antoni, B Långström.   

Abstract

Positron emission tomography (PET) following intravenous administration of beta-[11C]-L-DOPA provides a method of assessing regional cerebral uptake and utilization of levodopa. Cerebral levodopa kinetics in the rhesus monkey were investigated after the inhibition of catechol-O-methyltransferase (COMT) with RO 40-7592, and after coadministration of the peripheral aromatic L-amino acid decarboxylase (AADC) inhibitors benserazide and carbidopa. Pretreatment with RO 40-7592 (10 mg/kg), benserazide (10 mg/kg) or carbidopa (3.5 mg/kg) did not change striatal k3, which mainly reflects the ability for the brain tissue to convert [11C]-L-DOPA to [11 C]-dopamine, although the brain's uptake of radioactivity increased substantially after pretreatment with the AADC inhibitors. When benserazide was coadministered with RO 40-7592 (10 mg/kg) a dose-dependent decrease in striatal k3 was measured with an apparent ED50 of 3 mg/kg. No such effect was indicated after pretreatment with the combination of RO 40-7592 (10 mg/kg) and carbidopa (3.5 mg/kg). The possible negative interactions of coadministration with COMT inhibitors and predominantly peripherally acting AADC inhibitors must be considered when used in the therapy of Parkinson's disease.

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Year:  1991        PMID: 1867835     DOI: 10.1007/bf01244653

Source DB:  PubMed          Journal:  J Neural Transm Gen Sect


  13 in total

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Journal:  J Neurol Neurosurg Psychiatry       Date:  1989-06       Impact factor: 10.154

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Authors:  J Tedroff; S M Aquilonius; P Hartvig; H Lundqvist; P Bjurling; B Långström
Journal:  Acta Neurol Scand       Date:  1992-03       Impact factor: 3.209

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Journal:  Am J Physiol       Date:  1971-12

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Journal:  Pharmacol Rev       Date:  1966-03       Impact factor: 25.468

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Authors:  J G Nutt
Journal:  Ann Neurol       Date:  1987-10       Impact factor: 10.422

8.  Benserazide and carbidopa as substrates of catechol-O-methyltransferase: new mechanism of action in Parkinson's disease.

Authors:  R M Hagan; M J Raxworthy; P A Gulliver
Journal:  Biochem Pharmacol       Date:  1980-12-01       Impact factor: 5.858

9.  Purification and kinetic mechanism of human brain soluble catechol-O-methyltransferase.

Authors:  D R Jeffery; J A Roth
Journal:  J Neurochem       Date:  1985-03       Impact factor: 5.372

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Authors:  P Hartvig; H Agren; L Reibring; J Tedroff; P Bjurling; T Kihlberg; B Långström
Journal:  J Neural Transm Gen Sect       Date:  1991
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  4 in total

Review 1.  Clinical pharmacology, therapeutic use and potential of COMT inhibitors in Parkinson's disease.

Authors:  S Kaakkola
Journal:  Drugs       Date:  2000-06       Impact factor: 9.546

2.  Clinical Potential of Catechol-OMethyltransferase (COMT) Inhibitors as Adjuvants in Parkinson's Disease.

Authors:  P T Ménnistó
Journal:  CNS Drugs       Date:  1994-03       Impact factor: 5.749

3.  Antiparkinsonian Agents : Clinically Significant Drug Interactions and Adverse Effects, and Their Management.

Authors:  A Dalvi; B Ford
Journal:  CNS Drugs       Date:  1998-04       Impact factor: 5.749

4.  Regional brain kinetics of 6-fluoro-(beta-11C)-L-dopa and (beta-11C)-L-dopa following COMT inhibition. A study in vivo using positron emission tomography.

Authors:  P Hartvig; K J Lindner; J Tedroff; P Bjurling; K Hörnfelt; B Långström
Journal:  J Neural Transm Gen Sect       Date:  1992
  4 in total

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