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Structure of HIV-2 reverse transcriptase at 2.35-A resolution and the mechanism of resistance to non-nucleoside inhibitors

机译:HIV-2逆转录酶在2.35-A分辨率下的结构及其对非核苷抑制剂的耐药机制

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The HIV-2 serotype of HIV is a cause of disease in parts of the West African population, and there is evidence for its spread to Europe and Asia. HIV-2 reverse transcriptase (RT) demonstrates an intrinsic resistance to non-nucleoside RT inhibitors (NNRTIs), one of two classes of anti-AIDS drugs that target the viral RT. We report the crystal structure of HIV-2 RT to 2.35 A resolution, which reveals molecular details of the resistance to NNRTIs. HIV-2 RT has a similar overall fold to HIV-1 RT but has structural differences within the "NNRTI pocket" at both conserved and nonconserved residues. The structure points to the role of sequence differences that can give rise to unfavorable inhibitor contacts or destabilization of part of the binding pocket at positions 101, 106, 138, 181, 188, and 190. We also present evidence that the conformation of Ile-181 compared with the HIV-1 Tyr-181 could be a significant contributory factor to this inherent drug resistance of HIV-2 to NNRTIs. The availability of a refined structure of HIV-2 RT will provide a stimulus for the structure-based design of novel non-nucleoside inhibitors that could be used against HIV-2 infection.
机译:HIV-2血清型的HIV在西非部分人口中是引起疾病的原因,并且有证据表明它已传播到欧洲和亚洲。 HIV-2逆转录酶(RT)表现出对非核苷RT抑制剂(NNRTIs)的内在抗性,NNRTIs是针对病毒RT的两类抗艾滋病药物之一。我们报告到2.35 A分辨率的HIV-2 RT的晶体结构,揭示了抗NNRTIs的分子细节。 HIV-2 RT具有与HIV-1 RT相似的总体折叠率,但在“ NNRTI口袋”内的保守和非保守残基均具有结构差异。该结构指出了序列差异的作用,该差异可能导致不利的抑制剂接触或在101、106、138、181、188和190位的结合口袋部分不稳定。我们还提供了Ile-与HIV-1 Tyr-181相比,181可能是HIV-2对NNRTIs固有耐药性的重要因素。 HIV-2 RT的精制结构的可用性将为可用于抗HIV-2感染的新型非核苷抑制剂的基于结构的设计提供刺激。

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