Pyrrolobenzothiazepinones and pyrrolobenzoxazepinones: Novel and specific non-nucleoside HIV-1 reverse transcriptase inhibitors with antiviral activity

被引：48

作者：

Campiani, G

Nacci, V

Fiorini, I

DeFilippis, MP

Garofalo, A

Greco, G

Novellino, E

Altamura, S

DiRenzo, L

机构：

[1] UNIV SIENA, DIPARTIMENTO FARMACO CHIM TECNOL, I-53100 SIENA, ITALY

[2] UNIV NAPLES FEDERICO II, DIPARTIMENTO CHIM FARMACEUT & TOSSICOL, I-80131 NAPLES, ITALY

[3] IST RIC BIOL MOLEC P ANGELETTI, I-00040 Monte Porzio Catone, ITALY

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 1996年 / 39卷 / 14期

关键词：

D O I：

10.1021/jm950702c

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Two novel classes of pyrrolobenzothiazepinones and pyrrolobenzoxazepinones were investigated as potential anti-AIDS drugs. These compounds were found to inhibit HIV-1 reverse transcriptase (RT) enzyme in vitro and to prevent HIV-1 cytopathogenicity in T4 lymphocytes, without appreciable activity on HIV-2 cytopathic effects, and against HBV as well as calf-thymus DNA alpha-polymerase. Their potency is influenced by substituents at position 6 and on the fused aromatic ring. Specifically, small lipophilic substituents at C-6 were preferred, whereas substitutions on the benzo-fused ring were found to be detrimental to activity, with respect to the unsubstituted compounds. Modification of the pi-system at C-6 is well tolerated, although the replacement of the benzo-fused with a [2,3]naphtho-fused ring leads to a less active compound. Maximum potency and specificity is achieved with a phenyl and an ethyl group at position 6 of the pyrrolobenzoxazepinone system. In the enzymatic assay the oxazepinone derivative (+/-)-6-ethyl-6-phenylpyrrolo[2,1-d][1,5] 16e (IC50 = 0.25 mu M) was found to be more potent than nevirapine (IC50 = 0.5 mu M), tested in the same experimental conditions using rC . dG as a template-primer. In cell culture assay benzoxazepine 16e was active against HIV-1, both wild type and AZT-sensitive, and HIV-1 (IIIB) strains, but not against HIV-2. In enzyme assay although 16e inhibited HIV-1 RT, it was inactive against the nevirapine-resistant recombinant RT Y181C at 50 mu M. Molecular modeling studies suggest that these derivatives present a 3D pharmacophoric arrangement similar to that of other nonnucleoside inhibitors such as nevirapine.

引用

页码：2672 / 2680

页数：9

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