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1型人类免疫缺陷病毒逆转录酶抑制剂作用于早期逆转录的不同阶段。

Inhibitors of human immunodeficiency virus type 1 reverse transcriptase target distinct phases of early reverse transcription.

作者信息

Hooker C W, Lott W B, Harrich D

机构信息

HIV-1 and Hepatitis C Units, Sir Albert Sakzewski Virus Research Centre, Royal Children's Hospital, Herston, St. Lucia, Queensland, Australia.

出版信息

J Virol. 2001 Apr;75(7):3095-104. doi: 10.1128/JVI.75.7.3095-3104.2001.

Abstract

Early HIV-1 reverse transcription can be separated into initiation and elongation phases. Here we show, using PCR analysis of negative-strand strong-stop DNA [(-)ssDNA] synthesis in intact virus, that different reverse transcriptase (RT) inhibitors affect distinct phases of early natural endogenous reverse transcription (NERT). The effects of nevirapine on NERT were consistent with a mechanism of action including both specific and nonspecific binding events. The nonspecific component of this inhibition targeted the elongation reaction, whereas the specific effect seemed principally to be directed at very early events (initiation or the initiation-elongation switch). In contrast, foscarnet and the nucleoside analog ddATP inhibited both early and late (-)ssDNA synthesis in a similar manner. We also examined compounds that targeted other viral proteins and found that Ro24-7429 (a Tat antagonist) and rosmarinic acid (an integrase inhibitor) also directly inhibited RT. Our results indicate that NERT can be used to identify and evaluate compounds that directly target the reverse transcription complex.

摘要

早期HIV-1逆转录可分为起始阶段和延伸阶段。在此,我们通过对完整病毒中负链强终止DNA[(-)ssDNA]合成进行PCR分析表明,不同的逆转录酶(RT)抑制剂影响早期自然内源性逆转录(NERT)的不同阶段。奈韦拉平对NERT的作用符合一种作用机制,包括特异性和非特异性结合事件。这种抑制的非特异性成分靶向延伸反应,而特异性作用似乎主要针对非常早期的事件(起始或起始-延伸转换)。相比之下,膦甲酸和核苷类似物ddATP以类似方式抑制早期和晚期(-)ssDNA合成。我们还研究了靶向其他病毒蛋白的化合物,发现Ro24-7429(一种Tat拮抗剂)和迷迭香酸(一种整合酶抑制剂)也直接抑制RT。我们的结果表明,NERT可用于鉴定和评估直接靶向逆转录复合物的化合物。

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