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具有旨在最大化抗体依赖性细胞毒性的N-聚糖的均一IgG-Fc糖型的晶体结构。

Crystal Structure of a Homogeneous IgG-Fc Glycoform with the N-Glycan Designed to Maximize the Antibody Dependent Cellular Cytotoxicity.

作者信息

Chen Chia-Lin, Hsu Jen-Chi, Lin Chin-Wei, Wang Chia-Hung, Tsai Ming-Hung, Wu Chung-Yi, Wong Chi-Huey, Ma Che

机构信息

Genomics Research Center, Academia Sinica , Taipei, Taiwan.

Chemical Biology and Molecular Biophysics program, Taiwan International Graduate Program, Academia Sinica , Taipei, Taiwan.

出版信息

ACS Chem Biol. 2017 May 19;12(5):1335-1345. doi: 10.1021/acschembio.7b00140. Epub 2017 Mar 31.

DOI:10.1021/acschembio.7b00140
PMID:28318221
Abstract

N-glycosylation on IgG modulates Fc conformation and effector functions. An IgG-Fc contains a human sialo-complex type (hSCT) glycan of biantennary structure with two α2,6-sialylations and without core-fucosylation is an optimized glycoform developed to enhance the antibody dependent cellular cytotoxicity (ADCC). hSCT modification not only enhances the binding affinity to Fc receptors in the presence of antigen but also in some cases provides gain-of-function effector activity. We used enzymatic glyco-engineering to prepare an IgG-Fc with homogeneous hSCT attached to each C2 domain and solved its crystal structure. A compact form and an open form were observed in an asymmetric unit in the crystal. In the compact structure, the double glycan latches from the two hSCT chains stabilize the C2 domains in a closed conformation. In the open structure, the terminal sialic acid (N-acetylneuraminic acid or NeuNAc) residue interacts through water-mediated hydrogen bonds with the D249-L251 helix, to modulate the pivot region of the C2-C3 interface. The double glycan latches and the sialic acid modulation may be mutually exclusive. This is the first crystal structure of glyco-engineered Fc with enhanced effector activities. This work provides insights into the relationship between the structural stability and effector functions affected by hSCT modification and the development of better antibodies for therapeutic applications.

摘要

IgG上的N-糖基化调节Fc构象和效应功能。一种IgG-Fc含有具有双天线结构的人唾液酸复合类型(hSCT)聚糖,带有两个α2,6-唾液酸化且无核心岩藻糖基化,是为增强抗体依赖性细胞毒性(ADCC)而开发的优化糖型。hSCT修饰不仅在存在抗原的情况下增强与Fc受体的结合亲和力,而且在某些情况下还提供功能获得性效应活性。我们使用酶促糖工程制备了一种IgG-Fc,其每个C2结构域都连接有均一的hSCT,并解析了其晶体结构。在晶体的不对称单元中观察到一种紧密形式和一种开放形式。在紧密结构中,来自两条hSCT链的双聚糖锁扣将C2结构域稳定在封闭构象中。在开放结构中,末端唾液酸(N-乙酰神经氨酸或NeuNAc)残基通过水介导的氢键与D249-L251螺旋相互作用,以调节C2-C3界面的枢纽区域。双聚糖锁扣和唾液酸调节可能相互排斥。这是具有增强效应活性的糖工程化Fc的首个晶体结构。这项工作为受hSCT修饰影响的结构稳定性与效应功能之间的关系以及开发用于治疗应用的更好抗体提供了见解。

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