Small-molecule HIV-1 integrase inhibitors: the 2001-2002 update

被引:76
|
作者
Dayam, R [1 ]
Neamati, N [1 ]
机构
[1] Univ So Calif, Sch Pharm, Dept Pharmaceut Sci, Los Angeles, CA 90089 USA
关键词
HIV-1; integrase; structure-based drug design; inhibitors; drug discovery; S-1360; 5-CITEP;
D O I
10.2174/1381612033454469
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Integration of viral DNA into host cell chromosomal DNA to form a provirus is an essential step in the viral life cycle. This process is mediated by integrase (IN), a 32 KDa viral enzyme. The unique properties of IN makes it an ideal target for drug design. First, there are no cellular homologues to IN and the reactions catalyzed by IN are unique. Second, IN is absolutely required for viral replication and mutations in a number of key residues dramatically block viral replication. Third, IN has been validated as a legitimate target and the results from S-1360 (1) the only available IN inhibitor under clinical trials suggest synergistic effect with reverse transcriptase (RT) and protease (PR) inhibitors. During the past 10 years a plethora of inhibitors have been identified and some were shown to be selective against IN and block viral replication. The two most predominant classes of inhibitors have been the catechol containing hydroxylated aromatics and more recently the diketoacid containing aromatics. Herein, we review all small molecule compounds reported to inhibit recombinant HIV-1 IN with IC50 values < 20 mu M during the past two years. It is important to bear in mind that the true mechanism of action and antiviral activities of many of the compounds are currently not established. However, based on the growing body of literature certain classes Of compounds can be easily excluded as bona fide IN inhibitors.
引用
收藏
页码:1789 / 1802
页数:14
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