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一种合成潜在金属螯合TSAO-T衍生物作为1型人类免疫缺陷病毒逆转录酶双齿抑制剂的方法。

An approach towards the synthesis of potential metal-chelating TSAO-T derivatives as bidentate inhibitors of human immunodeficiency virus type 1 reverse transcriptase.

作者信息

Chamorro C, Camarasa M J, Pérez-Pérez M J, de Clercq E, Balzarini J, San Félix A

机构信息

Instituto de Química Médica (CSIC), Madrid, Spain.

出版信息

Antivir Chem Chemother. 1998 Sep;9(5):413-22.

PMID:9875394
Abstract

Novel derivatives of the potent human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT) inhibitor TSAO-T have been designed, synthesized and tested for their in vitro antiretroviral activity against HIV. These TSAO-T derivatives have been designed as potential bidentate inhibitors of HIV-1 RT, which combine in their structure the functionality of a non-nucleoside RT inhibitor (TSAO-T) and a bivalent ion-chelating moiety (a beta-diketone moiety) linked through an appropriate spacer to the N-3 of thymine of TSAO-T. Some of the new compounds have an anti-HIV-1 activity comparable to that of the parent compound TSAO-T, but display a markedly increased antiviral selectivity. There was a clear relationship between antiviral activity and the length of the spacer group that links the TSAO molecule with the chelating moiety. A shorter spacer invariably resulted in increased antiviral potency. None of the TSAO-T derivatives were endowed with anti-HIV-2 activity.

摘要

已设计、合成并测试了强效人类免疫缺陷病毒1型(HIV-1)逆转录酶(RT)抑制剂TSAO-T的新型衍生物,以评估它们对HIV的体外抗逆转录病毒活性。这些TSAO-T衍生物被设计为HIV-1 RT的潜在双齿抑制剂,其结构结合了非核苷RT抑制剂(TSAO-T)的功能和通过合适间隔基团连接到TSAO-T胸腺嘧啶N-3位的二价离子螯合部分(β-二酮部分)。一些新化合物具有与母体化合物TSAO-T相当的抗HIV-1活性,但显示出明显提高的抗病毒选择性。抗病毒活性与连接TSAO分子和螯合部分的间隔基团长度之间存在明确关系。较短的间隔基团总是导致抗病毒效力增加。没有一种TSAO-T衍生物具有抗HIV-2活性。

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4"-H-TSAO-T, a novel prototype in the HIV-1 specific TSAO family.4"-H-TSAO-T,HIV-1特异性TSAO家族中的一种新型原型。
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