Stereochemical Aspects of the anti-HCMV Activity of Cytidine Nucleoside Analogues

Author:

Mansour T. S.,Cimpoia A. R.1,Jin H.1,Hunter P. J.1,Evans C. A.1,Tse H. L. A.1,Gillard J. W.1,Borthwick A. D.2,Knight D. J.2,Coates J. A. V.2

Affiliation:

1. BioChem Therapeutic Inc., 275 Armand-Frappier Boulevard, Laval (Quebec), H7V 4A7, Canada

2. Glaxo Research and Development Ltd., Greenford Road, Greenford, Middlesex UB6 OHE, UK

Abstract

The remarkable selectivity of the β-L enantiomers of 2′,3′-dideoxycytidine analogues against the viral polymerases of HIV and HBV has stimulated our interest in targeting β-L enantiomers of anti-HCMV cytidine analogues. Indeed, Ara-C, FIAC and DMDC are cytidine analogues with β-D configuration that show significant potency as anti-HCMV agents but lack selectivity. β-L enantiomers have therefore been synthesized and evaluated together with four other nucleoside analogues, and the β-L. enantiomers were found not to be inhibitory to HCMV replication. However, the three α-L isomers, α-L-Ara-C, α-L-Xylo-C and α-L-FMAU, emerged with activity against HCMV and have provided new approaches for the treatment of viral diseases with nucleoside analogues possessing the unusual L-configuration.

Publisher

SAGE Publications

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