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Small-angle X-ray characterization of the nucleoprotein complexes resulting from DNA-induced oligomerization of HIV-1 integrase

机译:DNA诱导的HIV-1整合酶寡聚导致的核蛋白复合物的小角度X射线表征

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摘要

HIV-1 integrase (IN) catalyses integration of a DNA copy of the viral genome into the host genome. Specific interactions between retroviral IN and long terminal repeats (LTR) are required for this insertion. To characterize quantitatively the influence of the determinants of DNA substrate specificity on the oligomerization status of IN, we used the small-angle X-ray scattering (SAXS) technique. Under certain conditions in the absence of ODNs IN existed only as monomers. IN preincubation with specific ODNs led mainly to formation of dimers, the relative amount of which correlated well with the increase in the enzyme activity in the 3'-processing reaction. Under these conditions, tetramers were scarce. Non-specific ODNs stimulated formation of catalytically inactive dimers and tetramers. Complexes of monomeric, dimeric and tetrameric forms of IN with specific and non-specific ODNs had varying radii of gyration (R-g), suggesting that the specific sequence-dependent formation of IN tetramers can probably occur by dimerization of two dimers of different structure. From our data we can conclude that the DNA-induced oligomerization of HIV-1 IN is probably of importance to provide substrate specificity and to increase the enzyme activity.
机译:HIV-1整合酶(IN)催化将病毒基因组的DNA拷贝整合到宿主基因组中。逆转录病毒IN和长末端重复序列(LTR)之间需要特定的相互作用才能插入。为了定量表征DNA底物特异性决定因素对IN寡聚化状态的影响,我们使用了小角度X射线散射(SAXS)技术。在不存在ODN的某些条件下,IN仅作为单体存在。在与特定ODN的预温育中,主要导致二聚体的形成,二聚体的相对量与3'加工反应中酶活性的增加密切相关。在这些条件下,四聚体是稀缺的。非特异性ODN刺激了催化惰性二聚体和四聚体的形成。 IN的单体,二聚体和四聚体形式与特定和非特定ODN的复合物具有不同的回转半径(R-g),这表明IN四聚体的特定序列依赖性形成可能通过不同结构的两个二聚体的二聚作用发生。根据我们的数据,我们可以得出结论,DNA诱导的HIV-1 IN寡聚可能对提供底物特异性和增加酶的活性很重要。

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