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Impact of glycan cloud on the B-cell epitope prediction of SARS-CoV-2 Spike protein

机译:聚糖云对SARS-COV-2穗蛋白B细胞表位预测的影响

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The SARS-CoV-2 outbreak originated in China in late 2019 and has since spread to pandemic proportions. Diagnostics, therapeutics and vaccines are urgently needed. We model the trimeric Spike protein, including flexible loops and all N-glycosylation sites, in order to elucidate accessible epitopes for antibody-based diagnostics, therapeutics and vaccine development. Based on published experimental data, six homogeneous glycosylation patterns and two heterogeneous ones were used for the analysis. The glycan chains alter the accessible surface areas on the S-protein, impeding antibody-antigen recognition. In presence of glycan, epitopes on the S1 subunit, that notably contains the receptor binding domain, remain mostly accessible to antibodies while those present on the S2 subunit are predominantly inaccessible. We identify 28 B-cell epitopes in the Spike structure and group them as non-affected by the glycan cloud versus those which are strongly masked by the glycan cloud, resulting in a list of favourable epitopes as targets for vaccine development, antibody-based therapy and diagnostics.
机译:2019年底,SARS-COV-2爆发起源于中国,此后蔓延到大流行比例。迫切需要诊断,治疗和疫苗。我们模拟三聚体尖峰蛋白,包括柔性环和所有N-糖基化位点,以阐明基于抗体的诊断,治疗和疫苗发育的可偏离表位。基于已发表的实验数据,使用六种均匀的糖基化图案和两个异质糖基,用于分析。聚糖链改变了S蛋白的可移表面区域,阻碍抗体 - 抗原识别。在甘草存在下,S1亚基的表位,显着含有受体结合结构域,仍然可以易于抗体,而S2亚基的那些主要是不可接受的。我们鉴定尖峰结构中的28个B细胞表位,并将其分组为受甘油云强烈掩盖的甘油云影响,导致良好的表位列表作为疫苗发育的靶标,基于抗体的疗法和诊断。

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