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本文引用的文献

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Glycosylation of Fcγ receptors influences their interaction with various IgG1 glycoforms.Fcγ 受体的糖基化影响其与各种 IgG1 糖型的相互作用。
Mol Immunol. 2020 May;121:144-158. doi: 10.1016/j.molimm.2020.03.010. Epub 2020 Mar 26.
2
On-Membrane Dynamic Interplay between Anti-GM1 IgG Antibodies and Complement Component C1q.抗 GM1 IgG 抗体与补体成分 C1q 间的膜上动态相互作用
Int J Mol Sci. 2019 Dec 24;21(1):147. doi: 10.3390/ijms21010147.
3
Antibody Structure and Function: The Basis for Engineering Therapeutics.抗体结构与功能:工程治疗学的基础。
Antibodies (Basel). 2019 Dec 3;8(4):55. doi: 10.3390/antib8040055.
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IgG Antibody 3D Structures and Dynamics.IgG抗体的三维结构与动力学
Antibodies (Basel). 2018 Apr 19;7(2):18. doi: 10.3390/antib7020018.
5
Dynamic Views of the Fc Region of Immunoglobulin G Provided by Experimental and Computational Observations.实验与计算观察提供的免疫球蛋白G Fc区的动态视图
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6
The Fab portion of immunoglobulin G contributes to its binding to Fcγ receptor III.免疫球蛋白 G 的 Fab 部分有助于其与 Fcγ 受体 III 的结合。
Sci Rep. 2019 Aug 16;9(1):11957. doi: 10.1038/s41598-019-48323-w.
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Unraveling the Macromolecular Pathways of IgG Oligomerization and Complement Activation on Antigenic Surfaces.揭示抗原表面 IgG 寡聚化和补体激活的大分子途径。
Nano Lett. 2019 Jul 10;19(7):4787-4796. doi: 10.1021/acs.nanolett.9b02220. Epub 2019 Jun 11.
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Characterizing the Diversity of the CDR-H3 Loop Conformational Ensembles in Relationship to Antibody Binding Properties.表征 CDR-H3 环构象集合与抗体结合特性的关系的多样性。
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9
Structure and Dynamics of Immunoglobulin G Glycoproteins.免疫球蛋白 G 糖蛋白的结构与动态
Adv Exp Med Biol. 2018;1104:219-235. doi: 10.1007/978-981-13-2158-0_11.
10
Stable isotope labeling approaches for NMR characterization of glycoproteins using eukaryotic expression systems.使用真核表达系统对糖蛋白进行核磁共振表征的稳定同位素标记方法。
J Biomol NMR. 2018 Jul;71(3):193-202. doi: 10.1007/s10858-018-0169-2. Epub 2018 Feb 28.

免疫球蛋白G动态结构的生物物理特性分析

Biophysical characterization of dynamic structures of immunoglobulin G.

作者信息

Yanaka Saeko, Yogo Rina, Kato Koichi

机构信息

Exploratory Research Center on Life and Living Systems (ExCELLS) and Institute for Molecular Science (IMS), National Institutes of Natural Sciences, 5-1 Higashiyama, Myodaiji, Okazaki, 444-8787, Japan.

Graduate School of Pharmaceutical Sciences, Nagoya City University, 3-1 Tanabe-dori, Mizuho-ku, Nagoya, Aichi, 467-8603, Japan.

出版信息

Biophys Rev. 2020 Jun;12(3):637-645. doi: 10.1007/s12551-020-00698-1. Epub 2020 May 15.

DOI:10.1007/s12551-020-00698-1
PMID:32410186
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7311591/
Abstract

Immunoglobulin G (IgG) is a major antibody and functions as a hub linking specific antigen binding and recruitment of effector molecules typified by Fcγ receptors (FcγRs). These activities are associated primarily with interactions involving its Fab and Fc sites, respectively. An IgG molecule is characterized by a multiple domain modular structure with conserved N-glycosylation in Fc. The molecule displays significant freedom in internal motion on various spatiotemporal scales. The consequent conformational flexibility and plasticity of IgG glycoproteins are functionally significant and potentially important factors for design and engineering of antibodies with enhanced functionality. In this article, experimental and computational approaches are outlined for characterizing the conformational dynamics of IgG molecules in solution. In particular, the importance of integration of these approaches is highlighted, as illustrated by dynamic intramolecular interactions between the pair of N-glycans and their proximal amino acid residues in Fc. These interactions can critically affect effector functions mediated by human IgG1 and FcγRIII. Further improvements in individual biophysical techniques and their integration will advance understanding of dynamic behaviors of antibodies in physiological and pathological conditions. Such understanding will provide opportunities for engineering antibodies through controlling allosteric networks in IgG molecules.

摘要

免疫球蛋白G(IgG)是一种主要抗体,作为连接特异性抗原结合和以Fcγ受体(FcγRs)为代表的效应分子募集的枢纽发挥作用。这些活性分别主要与涉及其Fab和Fc位点的相互作用相关。IgG分子的特征是具有多结构域模块化结构,Fc中存在保守的N-糖基化。该分子在各种时空尺度上的内部运动表现出显著的自由度。IgG糖蛋白随之而来的构象灵活性和可塑性在功能上具有重要意义,并且是设计和工程化具有增强功能的抗体的潜在重要因素。在本文中,概述了用于表征溶液中IgG分子构象动力学的实验和计算方法。特别强调了整合这些方法 的重要性,Fc中一对N-聚糖与其近端氨基酸残基之间的动态分子内相互作用对此进行了说明。这些相互作用可严重影响人IgG1和FcγRIII介导的效应功能。个体生物物理技术及其整合的进一步改进将推动对抗体在生理和病理条件下动态行为的理解。这种理解将为通过控制IgG分子中的变构网络来工程化抗体提供机会。