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沙贝科病毒 RBD 缺失和特定残基决定了多物种 ACE2 的适应性。

Sarbecovirus RBD indels and specific residues dictating multi-species ACE2 adaptiveness.

机构信息

State Key Laboratory of Virology, College of Life Sciences, TaiKang Center for Life and Medical Sciences, Wuhan University, Wuhan, Hubei, China.

Wuhan Institute of Virology, Chinese Academy of Sciences, Wuhan, China.

出版信息

Nat Commun. 2024 Oct 14;15(1):8869. doi: 10.1038/s41467-024-53029-3.

Abstract

Our comprehensive understanding of the multi-species ACE2 adaptiveness of sarbecoviruses remains elusive, particularly for those with various receptor binding motif (RBM) insertions/deletions (indels). Here, we analyzed RBM sequences from 268 sarbecoviruses categorized into four RBM indel types. We examined the ability of 20 representative sarbecovirus Spike glycoproteins (S) and derivatives in utilizing ACE2 from various bats and several other mammalian species. We reveal that sarbecoviruses with long RBMs (type-I) can achieve broad ACE2 tropism, whereas viruses with single deletions in Region 1 (type-II) or Region 2 (type-III) exhibit narrower ACE2 tropism. Sarbecoviruses with double region deletions (type-IV) completely lost ACE2 usage, which is restricted by clade-specific residues within and outside RBM. Lastly, we propose the evolution of sarbecovirus RBM indels and illustrate how loop lengths, disulfide, and residue determinants shape multi-species ACE2 adaptiveness. This study provides profound insights into the mechanisms governing ACE2 usage and spillover risks of sarbecoviruses.

摘要

我们对沙贝病毒科多物种 ACE2 适应性的全面了解仍然难以捉摸,特别是对于那些具有各种受体结合基序(RBM)插入/缺失(indels)的病毒。在这里,我们分析了分为四种 RBM indel 类型的 268 种沙贝病毒科的 RBM 序列。我们检测了 20 种代表性沙贝病毒刺突糖蛋白(S)及其衍生物利用来自各种蝙蝠和其他几种哺乳动物物种的 ACE2 的能力。我们揭示了具有长 RBM(I 型)的沙贝病毒科可以实现广泛的 ACE2 嗜性,而在区域 1(II 型)或区域 2(III 型)中具有单个缺失的病毒表现出较窄的 ACE2 嗜性。具有双区域缺失(IV 型)的沙贝病毒科完全失去了 ACE2 的使用能力,这受到 RBM 内和外部特定残基的限制。最后,我们提出了沙贝病毒科 RBM indels 的进化,并说明了环长度、二硫键和残基决定因素如何塑造多物种 ACE2 适应性。这项研究深入了解了 ACE2 使用和沙贝病毒溢出风险的控制机制。

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