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Characterization of rare lens epithelium-derived growth factor/p75 genetic variants identified in HIV-1 long-term nonprogressors

机译:在HIV-1长期非进展者中鉴定出的罕见晶状体上皮衍生的生长因子/ p75基因变异

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OBJECTIVE: Lens epithelium-derived growth factor (LEDGF)/p75 is a cellular binding partner of HIV-1 integrase and a crucial cofactor for HIV-1 replication. Here, we study two LEDGF/p75 exonic variants I436S and T473I, identified in HIV-1 long-term nonprogressors, together with Q472L. METHODS: In-vitro binding assays, cell culture complementation, and functional rescue. RESULTS: Binding affinities of wild-type, I436S, T473I, and Q472L LEDGF/p75 for HIV-1 integrase were comparable. All LEDGF/p75 variants bound equally well to LEDGF/p75 interacting partners JPO2 and PogZ. In addition, HIV-1 replication was evaluated in human somatic LEDGF/p75-knockout cells and LEDGF/p75-knockdown cells complemented with either wild-type LEDGF/p75 or the respective LEDGF/p75 variants. All variants rescued HIV-1 replication to wild-type levels, whereas LEDGF/p75 D366N, defective for interaction with HIV-1 integrase, did not. CONCLUSION: Although identified in a cohort of long-term nonprogressors, our study did not indicate that the I436S or T473I mutation in LEDGF/p75 affects the interaction with HIV-1 integrase.
机译:目的:晶状体上皮细胞生长因子(LEDGF)/ p75是HIV-1整合酶的细胞结合伴侣,是HIV-1复制的关键辅助因子。在这里,我们研究了在HIV-1长期非进展者中发现的两个LEDGF / p75外显子变体I436S和T473I,以及Q472L。方法:体外结合测定,细胞培养互补和功能抢救。结果:野生型,I436S,T473I和Q472L LEDGF / p75对HIV-1整合酶的结合亲和力相当。所有LEDGF / p75变体均与LEDGF / p75相互作用的伙伴JPO2和PogZ结合良好。另外,在人体LEDGF / p75敲除细胞和补充有野生型LEDGF / p75或各自的LEDGF / p75变体的LEDGF / p75敲除细胞中评估HIV-1复制。所有变体均将HIV-1复制恢复至野生型水平,而与HIV-1整合酶相互作用存在缺陷的LEDGF / p75 D366N没有。结论:尽管在长期非进展人群中被发现,但我们的研究并未表明LEDGF / p75中的I436S或T473I突变会影响与HIV-1整合酶的相互作用。

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