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Competing Hydrophobic and Screened-Coulomb Interactions in Hepatitis B Virus Capsid Assembly

机译:在乙型肝炎病毒衣壳装配中竞争性疏水和库仑相互作用。

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摘要

Recent experiments show that, in the range from ∼15 to 45°C, an increase in the temperature promotes the spontaneous assembly into capsids of the Escherichia coli-expressed coat proteins of hepatitis B virus. Within that temperature interval, an increase in ionic strength up to five times that of standard physiological conditions also acts to promote capsid assembly. To explain both observations we propose an interaction of mean force between the protein subunits that is the sum of an attractive hydrophobic interaction, driving the self-assembly, and a repulsive electrostatic interaction, opposing the self-assembly. We find that the binding strength of the capsid subunits increases with temperature virtually independently of the ionic strength, and that, at fixed temperature, the binding strength increases with the square root of ionic strength. Both predictions are in quantitative agreement with experiment. We point out the similarities of capsid assembly in general and the micellization of surfactants. Finally we make plausible that electrostatic repulsion between the native core subunits of a large class of virus suppresses the formation in vivo of empty virus capsids, that is, without the presence of the charge-neutralizing nucleic acid.
机译:最近的实验表明,在约15至45°C的温度范围内,温度的升高会促进大肠杆菌表达的乙型肝炎病毒外壳蛋白的自发组装成衣壳。在该温度间隔内,离子强度的增加最多达到标准生理条件的五倍,也可促进衣壳的组装。为了解释这两个观察结果,我们提出了蛋白质亚基之间的平均力相互作用,该相互作用是驱动自组装的有吸引力的疏水相互作用和与自组装相反的排斥性静电相互作用的总和。我们发现,衣壳亚基的结合强度实际上随温度增加而与离子强度无关,并且在固定温度下,结合强度随离子强度的平方根增加。两种预测都与实验定量吻合。我们指出了衣壳装配和表面活性剂胶束化的相似之处。最后,我们认为,一类大型病毒的天然核心亚基之间的静电排斥作用会抑制体内空病毒衣壳的形成,也就是说,不存在电荷中和核酸。

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