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Nucleation and growth phases in the polymerization of coat and scaffolding subunits into icosahedral procapsid shells.

机译:外壳和脚手架亚基聚合成二十面体前壳体壳的成核和生长阶段。

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摘要

The polymerization of protein subunits into precursor shells empty of DNA is a critical process in the assembly of double-stranded DNA viruses. For the well-characterized icosahedral procapsid of phage P22, coat and scaffolding protein subunits do not assemble separately but, upon mixing, copolymerize into double-shelled procapsids in vitro. The polymerization reaction displays the characteristics of a nucleation limited reaction: a paucity of intermediate assembly states, a critical concentration, and kinetics displaying a lag phase. Partially formed shell intermediates were directly visualized during the growth phase by electron microscopy of the reaction mixture. The morphology of these intermediates suggests that assembly is a highly directed process. The initial rate of this reaction depends on the fifth power of the coat subunit concentration and the second or third power of the scaffolding concentration, suggesting that pentamer of coat protein and dimers or trimers of scaffolding protein, respectively, participate in the rate-limiting step.
机译:蛋白质亚基聚合成不含DNA的前体壳是双链DNA病毒组装中的关键过程。对于充分表征的噬菌体P22的二十面体前壳体,外壳蛋白和支架蛋白亚基不能单独组装,但是在混合后,在体外共聚成双壳前壳体。聚合反应显示出成核受限反应的特征:缺乏中间组装状态,临界浓度和动力学表现出滞后相。在生长阶段,通过反应混合物的电子显微镜可以直接看到部分形成的壳中间体。这些中间体的形态表明组装是高度指导的过程。该反应的初始速率取决于外壳亚基浓度的五次幂和支架浓度的第二次或三次幂,表明外壳蛋白的五聚体和支架蛋白的二聚体或三聚体分别参与限速步骤。 。

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