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新型流感病毒H7N9识别蛋白H7与聚糖细胞表面受体相互作用的核磁共振与分子动力学模拟

Nuclear Magnetic Resonance and Molecular Dynamics Simulation of the Interaction between Recognition Protein H7 of the Novel Influenza Virus H7N9 and Glycan Cell Surface Receptors.

作者信息

Macchi Eleonora, Rudd Timothy R, Raman Rahul, Sasisekharan Ram, Yates Edwin A, Naggi Annamaria, Guerrini Marco, Elli Stefano

机构信息

Istituto di Ricerche Chimiche e Biochimiche "G. Ronzoni" , Via Giuseppe Colombo 81, 20133 Milano, Italy.

National Institute for Biological Standards and Control (NIBSC) , Blanche Lane, South Mimms, Potters Bar, Hertfordshire EN6 3QG, U.K.

出版信息

Biochemistry. 2016 Dec 6;55(48):6605-6616. doi: 10.1021/acs.biochem.6b00693. Epub 2016 Nov 23.

DOI:10.1021/acs.biochem.6b00693
PMID:27933797
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5559875/
Abstract

Avian influenza A viruses, which can also propagate between humans, present serious pandemic threats, particularly in Asia. The specificity (selectivity) of interactions between the recognition protein hemagglutinin (HA) of the virus capsid and the glycoconjugates of host cells also contributes to the efficient spread of the virus by aerosol between humans. Some avian origin viruses, such as H1N1 (South Carolina 1918), have improved their selectivity for human receptors by mutation in the HA receptor binding site, to generate pandemic viruses. Molecular details and dynamics of glycan-HA interactions are of interest, both in predicting the pandemic potential of a new emerging strain and in searching for new antiviral drugs. Two complementary techniques, H saturation transfer difference (H STD) nuclear magnetic resonance and molecular dynamics (MD) simulation, were applied to analyze the interaction of the new H7 (A/Anhui/1/13 H7N9) with LSTa [Neu5Ac α(2→3) Gal β(1→3) GlcNAc β(1→3) Gal β(1→4) Glc] and LSTc [Neu5Ac α(2→6) Gal β(1→4) GlcNAc β(1→3) Gal β(1→4) Glc] pentasaccharides, models of avian and human receptor glycans. Their interactions with H7 were analyzed for the first time using H STD and MD, revealing structural and dynamic behavior that could not be obtained from crystal structures, and contributing to glycan-HA specificity. This highlighted aspects that could affect glycan-HA recognition, including the mutation H7 G228S, which increases H2 and H3 specificity for the human receptor. Finally, interactions between LSTc and H7 were compared with those between LSTc and H1 of H1N1 (South Carolina 1918), contributing to our understanding of the recognition ability of HAs.

摘要

甲型禽流感病毒也可在人与人之间传播,带来严重的大流行威胁,尤其是在亚洲。病毒衣壳识别蛋白血凝素(HA)与宿主细胞糖缀合物之间相互作用的特异性(选择性)也有助于病毒通过气溶胶在人与人之间有效传播。一些禽源病毒,如H1N1(南卡罗来纳州1918株),通过HA受体结合位点的突变提高了对人类受体的选择性,从而产生大流行病毒。聚糖-HA相互作用的分子细节和动力学,对于预测新出现毒株的大流行潜力以及寻找新的抗病毒药物都具有重要意义。两种互补技术,即1H饱和转移差(1H STD)核磁共振和分子动力学(MD)模拟,被用于分析新型H7(A/安徽/1/13 H7N9)与LSTa [Neu5Ac α(2→3)Gal β(1→3)GlcNAc β(1→3)Gal β(1→4)Glc]和LSTc [Neu5Ac α(2→6)Gal β(1→4)GlcNAc β(1→3)Gal β(1→4)Glc]五糖(禽源和人源受体聚糖模型)之间的相互作用。首次使用1H STD和MD分析了它们与H7的相互作用,揭示了从晶体结构中无法获得的结构和动力学行为,并有助于聚糖-HA特异性研究。这突出了可能影响聚糖-HA识别的方面,包括H7 G228S突变,该突变增加了H2和H3对人类受体的特异性。最后,将LSTc与H7之间的相互作用与LSTc与H1N1(南卡罗来纳州1918株)的H1之间的相互作用进行了比较,有助于我们理解HA的识别能力。

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