论文标题

Spike RBD的结合位点的低渗透保湿壳决定了SARS-COV-2变体的传染性

The low-entropy hydration shell at the binding site of spike RBD determines the contagiousness of SARS-CoV-2 variants

论文作者

Yang, Lin, Guo, Shuai, Houc, Chengyu, Lia, Jiacheng, Shi, Liping, Liao, Chenchen, Shi, Rongchun, Ma, Xiaoliang, Zheng, Bing, Fang, Yi, Ye, Lin, He, Xiaodong

论文摘要

SARS-COV-2的感染性取决于血管紧张素转化酶2(ACE2)受体的峰值蛋白的受体结合结构域(RBD)的结合亲和力。计算出的RBD-ACE2结合能表明,SARS-COV-2变体的传输效率差异无法通过静电相互作用,氢键相互作用,范德华相互作用,内部能量和非极性溶剂化能来完全解释。在这里,我们证明了蛋白质周围的水合壳的低渗透区域驱动水合壳的形状匹配的低透镜区域之间的疏水吸引力,这基本上是在相互方向的旋转式构造空间中的蛋白质 - 蛋白质结合,并确定结合亲和力。一种创新的方法用于识别多个SARS-COV-2变体和ACE2的RBD的水合壳的低渗透区域。我们观察到覆盖RBD的结合位点的水合壳的积分低渗透区域,并在ACE2的结合位点形状与水合壳的低渗透区匹配。因此,发现RBD-ACE2结合是由水合壳的形状匹配的低渗透区域之间的疏水性塌陷所指导的。可以通过计算在结合位点内表达亲水性的亲水基团的数量来获得水合壳的低渗透率的度量。发现尖峰蛋白结合位点的水合壳的低透镜水平被认为是冠状病毒传染性的重要指标。

The infectivity of SARS-CoV-2 depends on the binding affinity of the receptor-binding domain (RBD) of the spike protein with the angiotensin converting enzyme 2 (ACE2) receptor. The calculated RBD-ACE2 binding energies indicate that the difference in transmission efficiency of SARS-CoV-2 variants cannot be fully explained by electrostatic interactions, hydrogen-bond interactions, van der Waals interactions, internal energy, and nonpolar solvation energies. Here, we demonstrate that low-entropy regions of hydration shells around proteins drive hydrophobic attraction between shape-matched low-entropy regions of the hydration shells, which essentially coordinates protein-protein binding in rotational-configurational space of mutual orientations and determines the binding affinity. An innovative method was used to identify the low-entropy regions of the hydration shells of the RBDs of multiple SARS-CoV-2 variants and the ACE2. We observed integral low-entropy regions of hydration shells covering the binding sites of the RBDs and matching in shape to the low-entropy region of hydration shell at the binding site of the ACE2. The RBD-ACE2 binding is thus found to be guided by hydrophobic collapse between the shape-matched low-entropy regions of the hydration shells. A measure of the low-entropy of the hydration shells can be obtained by counting the number of hydrophilic groups expressing hydrophilicity within the binding sites. The low-entropy level of hydration shells at the binding site of a spike protein is found to be an important indicator of the contagiousness of the coronavirus.

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