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X-Ray Structures of the Hexameric Building Block of the HIV Capsid

机译:HIV衣壳六聚体构件的X射线结构

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The mature capsids of HIV and other retroviruses organize and package the viral genome and its associated enzymes for delivery into host cells. The HIV capsid is a fullerene cone: a variably curved, closed shell composed of approximately 250 hexamers and exactly 12 pentamers of the viral CA protein. We devised methods for isolating soluble, assembly-competent CA hexamers and derived four crystallographically independent models that define the structure of this capsid assembly unit at atomic resolution. A ring of six CA N-terminal domains form an apparently rigid core, surrounded by an outer ring of C-terminal domains. Mobility of the outer ring appears to be an underlying mechanism for generating the variably curved lattice in authentic capsids. Hexamer-stabilizing interfaces are highly hydrated, and this property may be key to the formation of quasi-equivalent interactions within hexamers and pentamers. The structures also clarify the molecular basis for capsid assembly inhibition and should facilitate structure-based drug design strategies.
机译:HIV和其他逆转录病毒的成熟衣壳组织并包装了病毒基因组及其相关酶,可传递到宿主细胞中。 HIV衣壳是一个富勒烯锥体:一个可变弯曲的封闭壳,由大约250个六聚体和恰好12个五聚体的病毒CA蛋白组成。我们设计了分离可溶性,可装配CA六聚体的方法,并推导了四个晶体学独立的模型,这些模型以原子分辨率定义了该衣壳装配单元的结构。六个CA N末端结构域的环形成一个明显刚性的核心,被C末端结构域的外环包围。外环的流动性似乎是在真实衣壳中产生可变弯曲晶格的潜在机制。六聚物稳定界面高度水合,并且该性质可能是六聚物和五聚物中拟等价相互作用形成的关键。该结构还阐明了衣壳装配抑制的分子基础,并应促进基于结构的药物设计策略。

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