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结合不同血凝素时禽源和人源唾液酸五糖受体类似物的独特聚糖拓扑结构:分子动力学视角

Distinct glycan topology for avian and human sialopentasaccharide receptor analogues upon binding different hemagglutinins: a molecular dynamics perspective.

作者信息

Xu Dong, Newhouse E Irene, Amaro Rommie E, Pao Hsing C, Cheng Lily S, Markwick Phineus R L, McCammon J Andrew, Li Wilfred W, Arzberger Peter W

机构信息

National Biomedical Computation Resource, University of California San Diego, La Jolla, CA 92093-0505, USA.

出版信息

J Mol Biol. 2009 Mar 27;387(2):465-91. doi: 10.1016/j.jmb.2009.01.040. Epub 2009 Feb 5.

Abstract

Hemagglutinin (HA) binds to sialylated glycans exposed on the host cell surface in the initial stage of avian influenza virus infection. It has been previously hypothesized that glycan topology plays a critical role in the human adaptation of avian flu viruses, such as the potentially pandemic H5N1. Comparative molecular dynamics studies are complementary to experimental techniques, including glycan microarray, to understand the mechanism of species-specificity switch better. The examined systems comprise explicitly solvated trimeric forms of avian H3, H5, and swine H9 in complex with avian and human glycan receptor analogues--LSTa (alpha-2,3-linked lactoseries tetrasaccharide a) and LSTc (alpha-2,6-linked lactoseries tetrasaccharide c), respectively. The glycans adopted distinct topological profiles with inducible torsional angles when bound to different HAs. The corresponding receptor binding domain amino acid contact profiles were also distinct. Avian H5 was able to accommodate LSTc in a tightly "folded umbrella"-like topology through interactions with all five sugar residues. After considering conformational entropy, the relative binding free-energy changes, calculated using the molecular mechanics-generalized Born surface area technique, were in agreement with previous experimental findings and provided insights on electrostatic, van der Waals, desolvation, and entropic contributions to HA-glycan interactions. The topology profile and the relative abundance of free glycan receptors may influence receptor binding kinetics. Glycan composition and topological changes upon binding different HAs may be important determinants in species-specificity switch.

摘要

血凝素(HA)在禽流感病毒感染的初始阶段与宿主细胞表面暴露的唾液酸化聚糖结合。此前有假说认为,聚糖拓扑结构在禽流感病毒适应人类的过程中起着关键作用,例如具有潜在大流行风险的H5N1病毒。比较分子动力学研究是对包括聚糖微阵列在内的实验技术的补充,有助于更好地理解物种特异性转换的机制。所研究的系统包括分别与禽类和人类聚糖受体类似物——LSTa(α-2,3连接的乳糖系列四糖a)和LSTc(α-2,6连接的乳糖系列四糖c)结合的禽类H3、H5和猪H9的明确溶剂化三聚体形式。当与不同的HA结合时,聚糖呈现出具有可诱导扭转角的不同拓扑结构。相应的受体结合域氨基酸接触图谱也各不相同。禽类H5能够通过与所有五个糖残基的相互作用,以紧密的“折叠伞”状拓扑结构容纳LSTc。在考虑构象熵后,使用分子力学-广义玻恩表面积技术计算的相对结合自由能变化与先前的实验结果一致,并提供了关于静电、范德华力、去溶剂化和熵对HA-聚糖相互作用贡献的见解。聚糖拓扑结构图谱和游离聚糖受体的相对丰度可能会影响受体结合动力学。结合不同HA时聚糖组成和拓扑结构的变化可能是物种特异性转换的重要决定因素。

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