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Integrase-RNA interactions underscore the critical role of integrase in HIV-1 virion morphogenesis

机译:Integrase-RNA相互作用强调整合酶在HIV-1 Viorion形态发生中的关键作用

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摘要

A large number of human immunodeficiency virus 1 (HIV-1) integrase (IN) alterations, referred to as class II substitutions, exhibit pleiotropic effects during virus replication. However, the underlying mechanism for the class II phenotype is not known. Here we demonstrate that all tested class II IN substitutions compromised IN-RNA binding in virions by one of the three distinct mechanisms: (i) markedly reducing IN levels thus precluding the formation of IN complexes with viral RNA; (ii) adversely affecting functional IN multimerization and consequently impairing IN binding to viral RNA; and (iii) directly compromising IN-RNA interactions without substantially affecting IN levels or functional IN multimerization. Inhibition of IN-RNA interactions resulted in the mislocalization of viral ribonucleoprotein complexes outside the capsid lattice, which led to premature degradation of the viral genome and IN in target cells. Collectively, our studies uncover causal mechanisms for the class II phenotype and highlight an essential role of IN-RNA interactions for accurate virion maturation.
机译:大量的人免疫缺陷病毒1(HIV-1)整合酶(IN)改变,称为II类取代,在病毒复制期间表现出脂肪熵作用。然而,II类表型的潜在机制是未知的。在这里,我们证明,通过三种不同机制之一通过其中一种在病毒粒子中损害的所有测试II类II,其中三种不同的机制之一:(i)在水平中显着降低,从而阻止与病毒RNA的复合物的形成; (ii)对多聚化的功能性产生不利影响,从而损害与病毒RNA的结合; (iii)直接损害RNA相互作用,而不会在多元化的水平或功能中没有影响。抑制RNA相互作用导致衣壳晶格外的病毒核糖核糖蛋白复合物的错误定位,其导致病毒基因组和靶细胞的过早降解。统称,我们的研究发现II类表型的因果机制,并突出了RNA相互作用的基本作用,以获得准确的病毒赛成熟。

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