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Inhibitors of the integrase–transportin-SR2 interaction block HIV nuclear import

机译:整合酶-转运蛋白-SR2相互作用的抑制剂可阻止艾滋病毒的核输入

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摘要

BackgroundCombination antiretroviral therapy efficiently suppresses HIV replication in infected patients, transforming HIV/AIDS into a chronic disease. Viral resistance does develop however, especially under suboptimal treatment conditions such as poor adherence. As a consequence, continued exploration of novel targets is paramount to identify novel antivirals that do not suffer from cross-resistance with existing drugs. One new promising class of targets are HIV protein–cofactor interactions. Transportin-SR2 (TRN-SR2) is a β-karyopherin that was recently identified as an HIV-1 cofactor. It has been implicated in nuclear import of the viral pre-integration complex and was confirmed as a direct binding partner of HIV-1 integrase (IN). Nevertheless, consensus on its mechanism of action is yet to be reached.
机译:背景联合抗逆转录病毒疗法可有效抑制感染患者的HIV复制,从而将HIV / AIDS转变为慢性疾病。但是,确实会产生病毒抗药性,特别是在治疗效果欠佳(例如依从性差)的情况下。因此,不断探索新的靶标对于鉴定不会与现有药物产生交叉耐药性的新型抗病毒药物至关重要。 HIV蛋白质-辅因子相互作用是一类新的有前景的靶标。 Transportin-SR2(TRN-SR2)是一种最近被鉴定为HIV-1辅助因子的β-karyopherin。它与病毒整合前复合物的核输入有关,并被证实是HIV-1整合酶(IN)的直接结合伴侣。然而,关于其作用机制尚待达成共识。

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