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2',3'-双脱氧核苷三磷酸对人免疫缺陷病毒逆转录酶的抑制作用:模板依赖性以及与膦甲酸的联合作用

Inhibition of human immunodeficiency virus reverse transcriptase by 2',3'-dideoxynucleoside triphosphates: template dependence, and combination with phosphonoformate.

作者信息

Starnes M C, Cheng Y C

机构信息

Department of Pharmacology, School of Medicine, University of North Carolina, Chapel Hill 27599.

出版信息

Virus Genes. 1989 May;2(3):241-51. doi: 10.1007/BF00125341.

Abstract

The 2',3'-dideoxynucleoside triphosphates (ddNTPs) are potent substrate analog inhibitors of human immunodeficiency virus (HIV) reverse transcriptase and have clinical utility in the treatment of acquired immunodeficiency syndrome. Several issues regarding the interaction of these compounds with HIV reverse transcriptase were examined. The potency of unsubstituted ddNTPs and the 3'-azido analog of dTTP (AZTTP) was influenced by the choice of template. Both compounds were more potent with the complementary homopolymer templates than with gapped duplex DNA, although the Km for the competing dNTP was similar with different templates. The Ki for AZTTP was greater than for the unsubstituted ddNTPs with either a homopolymer or a gapped duplex DNA template. HIV reverse transcriptase incorporated ddCMP and AZTMP into primed phage m13 DNA at sites specified for insertion of dCMP and dTMP, respectively. ddCTP was more efficiently utilized as a substrate than was AZTTP. Primer elongation due to base misincorporation was observed in the absence of one dNTP. The combined effect of ddNTPs and the pyrophosphate analog phosphonoformate (PFA) on HIV reverse transcriptase was also examined, and inhibition by PFA in combination with ddTTP or AZTTP was mutually exclusive.

摘要

2',3'-双脱氧核苷三磷酸(ddNTPs)是人类免疫缺陷病毒(HIV)逆转录酶的有效底物类似物抑制剂,在获得性免疫缺陷综合征的治疗中具有临床应用价值。研究了这些化合物与HIV逆转录酶相互作用的几个问题。未取代的ddNTPs和dTTP的3'-叠氮类似物(AZTTP)的效力受模板选择的影响。这两种化合物与互补同聚物模板的效力均高于与缺口双链DNA的效力,尽管竞争dNTP的Km在不同模板下相似。无论是同聚物模板还是缺口双链DNA模板,AZTTP的Ki均大于未取代的ddNTPs。HIV逆转录酶分别在指定插入dCMP和dTMP的位点将ddCMP和AZTMP掺入引发的噬菌体m13 DNA中。ddCTP作为底物的利用效率高于AZTTP。在缺少一种dNTP的情况下,观察到由于碱基错掺入导致的引物延伸。还研究了ddNTPs与焦磷酸类似物膦甲酸(PFA)对HIV逆转录酶的联合作用,PFA与ddTTP或AZTTP联合使用时的抑制作用相互排斥。

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