PMID: 10901289Jul 20, 2000Paper

The enantioselectivity of enzymes involved in current antiviral therapy using nucleoside analogues: a new strategy?

Antiviral Chemistry & Chemotherapy
G Maury

Abstract

This review is primarily intended for synthetic bio-organic chemists and enzymologists who are interested in new strategies in the design of virus inhibitors. It is an attempt to assess the importance of the enzymatic properties of L-nucleosides and their analogues, particularly those that are active against viruses such as human immunodeficiency virus (HIV), hepatitis B virus (HBV), herpes simplex virus (HSV), etc. Only data obtained with purified enzymes have been considered and discussed. The examined enzymes include nucleoside- or nucleotide-phosphorylating enzymes, catabolic enzymes, viral target enzymes and cellular polymerases. The enantioselectivities of these enzymes were determined from existing data and are significant only when a sufficient number of enantiomeric pairs of substrates could be examined. The reported data emphasize the weak enantioselectivities of cellular or viral nucleoside kinases and some viral DNA polymerases. Thus, cellular deoxycytidine kinase has a considerably relaxed enantioselectivity with respect to a large number of nucleosides or their analogues, and it occupies a strategic position in the intracellular activation of the compounds. Similarly, HIV-1 reverse transcriptase often has a relati...Continue Reading

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Citations

Dec 4, 2010·European Journal of Nuclear Medicine and Molecular Imaging·Johannes SchwarzenbergChristiaan Schiepers
Apr 16, 2003·European Journal of Biochemistry·Claudia PastiDominique Deville-Bonne
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