Inhibition of Human Cytomegalovirus Proteinase by Salcomine Derivatives

Author:

Watanabe S12,Konno K1,Shigeta S2,Yokota T1

Affiliation:

1. Rational Drug Design Laboratories, 4-1-1 Misato, Matsukawa-Machi, Fukushima 960–12, Japan

2. Department of Microbiology, Fukushima Medical College, 1 Hikarigaoka, Fukushima 960–12, Japan

Abstract

Salcomine, N,N'-bis(salicylidene)ethylene diaminocobalt (II), and its derivatives were evaluated for their ability to inhibit selectively human cytomegalovirus (HCMV) proteinase activity. The 50% inhibitory concentration (IC50) of salcomine was 1.4 μM for HCMV proteinase, but >200 μM for three other serine proteinases (trypsin, >250 μM; chymotrypsin, 206 μM; and elastase, >250 μM). Two salcomine derivatives also inhibited HCMV proteinase with IC50 values under 2 μM. Studies of the structure–activity relationship of salcomine-related compounds showed that the phenyl moiety and the spacer moiety (distance betweenthe two amines) were instrumental in the inhibition of HCMV proteinase. Moreover, salcomine inhibited the growth of laboratory strain AD169 and three clinical isolates at a 50% effective concentration (EC50) range of 1.92–2.89 μM. These results show that salcomine derivatives are potent and selective inhibitors of HCMV proteinase and HCMV replication in cell culture. Salcomine derivatives appear to be worth pursuing as candidate drugs for the chemotherapy of HCMV infection.

Publisher

SAGE Publications

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