Structure of the HIV-1 integrase catalytic domain complexed with an inhibitor: A platform for antiviral drug design

Yehuda Goldgur; Robert Craigie; Gerson H. Cohen; Tamio Fujiwara; Tomokazu Yoshinaga; Toshio Fujishita; Hirohiko Sugimoto; Takeshi Endo; Hitoshi Murai; David R. Davies

doi:10.1073/pnas.96.23.13040

Structure of the HIV-1 integrase catalytic domain complexed with an inhibitor: A platform for antiviral drug design

Yehuda Goldgur(National Institutes of Health), Robert Craigie(National Institutes of Health), Gerson H. Cohen(National Institutes of Health), Tamio Fujiwara(National Institutes of Health), Tomokazu Yoshinaga(National Institutes of Health), Toshio Fujishita(National Institutes of Health), Hirohiko Sugimoto(National Institutes of Health), Takeshi Endo(National Institutes of Health), Hitoshi Murai(National Institutes of Health), David R. Davies(National Institutes of Health)

Proceedings of the National Academy of Sciences

November 9, 1999

10.1073/pnas.96.23.13040

Cited by 494Open Access

Abstract

HIV integrase, the enzyme that inserts the viral DNA into the host chromosome, has no mammalian counterpart, making it an attractive target for antiviral drug design. As one of the three enzymes produced by HIV, it can be expected that inhibitors of this enzyme will complement the therapeutic use of HIV protease and reverse transcriptase inhibitors. We have determined the structure of a complex of the HIV-1 integrase core domain with a novel inhibitor, 5ClTEP, 1-(5-chloroindol-3-yl)-3-hydroxy-3-(2H-tetrazol-5-yl)-pro penone, to 2.1-A resolution. The inhibitor binds centrally in the active site of the integrase and makes a number of close contacts with the protein. Only minor changes in the protein accompany inhibitor binding. This inhibitor complex will provide a platform for structure-based design of an additional class of inhibitors for antiviral therapy.

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