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Inhibition of the integrases of human immunodeficiency viruses type 1 and type 2 by reverse transcriptases

机译:逆转录酶抑制1型和2型人类免疫缺陷病毒的整合

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pWe present evidence that the integrases (INs) of HIV types 1 and 2 are inhibited iin vitro/i by the reverse transcriptases (RTs) of HIV-1, HIV-2 and murine leukaemia virus. Both 3′-end processing and 3′-end joining (strand transfer) activities of IN were affected by the RTs. Full inhibitions were accomplished with most RT and IN combinations tested at around equimolar RT/IN ratios. The disintegration activity of IN was also inhibited by RTs. Neither DNA synthesis nor the ribonuclease H (RNase H) domain of RT were involved in IN inhibition, since specific DNA polymerase inhibitors did not affect the level of IN inhibition, and the p51 isoform of HIV-1 RT (which lacks the RNase H domain) is as effective in inhibiting IN as the heterodimeric p66/p51 isoform. On the other hand, the catalytic activities of HIV RTs were not affected by the INs, showing that RTs can inhibit IN activities, whereas INs do not inhibit RTs. We postulate that sequences and/or three-dimensional protein structures common to RTs interact with INs and inhibit their activities. We show evidence for this hypothesis and discuss the possible sites of IN involved in this interaction./p
机译:>我们提供的证据表明,HIV-1,HIV-2和鼠白血病病毒的逆转录酶(RTs)在体外抑制了1型和2型HIV的整合(IN)。 RT对IN的3'末端加工和3'末端结合(链转移)活性均产生影响。在大约等摩尔的RT / IN比下测试的大多数RT和IN组合均可实现完全抑制。 RT也抑制IN的崩解活性。 RT的DNA合成和核糖核酸酶H(RNase H)结构域均不参与IN抑制,因为特定的DNA聚合酶抑制剂不影响IN抑制的水平以及HIV-1 RT的p51亚型(缺少RNase H结构域) )在抑制IN方面与异二聚体p66 / p51亚型一样有效。另一方面,HIV RTs的催化活性不受INs的影响,表明RTs可以抑制INs的活性,而INs则不能抑制RTs。我们假设RT共有的序列和/或三维蛋白质结构与IN相互作用并抑制其活性。我们为该假设提供证据,并讨论了参与此相互作用的IN的可能位点。

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