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结构阐明初级体液免疫反应简并性的机制基础。

Structural elucidation of the mechanistic basis of degeneracy in the primary humoral response.

机构信息

Structural Biology Unit, National Institute of Immunology, New Delhi 110 067, India.

出版信息

J Immunol. 2012 Feb 15;188(4):1819-27. doi: 10.4049/jimmunol.1102701. Epub 2012 Jan 20.

DOI:10.4049/jimmunol.1102701
PMID:22266283
Abstract

The mechanistic basis for efficient combating of the infinite range of foreign Ags by the limited repertoire of naive Abs expressed on primary B cell surfaces during their first encounter was addressed through elegantly designed crystallographic analyses. Resolution of the discrepancy arising from the limited number of possible germline Ab receptors on primary B cells for recognizing the unlimited pool of possible Ags has been attempted by invoking the degenerate recognition potential of the germline Abs. Structural analyses of germline mAb BBE6.12H3 in an Ag-free state, as well as bound to four different peptide Ags, established the correlation of its degenerate specificity with conformational versatility of the paratope. Six distinct paratope topologies observed for a single germline mAb provided a quantitative description of the primary Ag recognition repertoire at the tertiary structural level. Each of the four different peptide Ags was bound specifically to a distinct conformation of the paratope, which was also different from that of the Ag-free states of the same germline mAb. A minimal conserved motif in the pristine Ag-combining site essential for multispecificity and Ag binding-mediated change in the elbow angle of Fab was also discernible. It is proposed that the generation of a primary Ab repertoire involves large, yet finite, germline Ab clones, each capable of adopting discrete conformations, which in turn exhibit diverse binding modes.

摘要

通过精心设计的晶体学分析,解决了在初级 B 细胞表面初次遇到时,由有限数量的幼稚 Abs 表达的有限 repertoire 高效对抗无限范围的外来 Ag 的机制基础。为了解决初级 B 细胞上用于识别无限数量可能的 Ag 的有限数量的 germline Ab 受体的问题,人们试图利用 germline Abs 的退化识别潜力。对无 Ag 状态下的 germline mAb BBE6.12H3 以及与四种不同肽 Ag 结合的结构分析,确立了其退化特异性与表位构象灵活性之间的相关性。单个 germline mAb 观察到的六种不同的表位拓扑结构,在三级结构水平上提供了对初级 Ag 识别 repertoire 的定量描述。四种不同的肽 Ag 中的每一种都特异性地结合到表位的独特构象,该构象也与相同 germline mAb 的无 Ag 状态不同。在原始 Ag 结合位点中,也可以识别到一个最小的保守基序,该基序对于多特异性和 Ag 结合介导的 Fab 肘角变化至关重要。有人提出,初级 Ab repertoire 的产生涉及到大量但有限的 germline Ab 克隆,每个克隆都能够采用离散的构象,而这些构象又表现出不同的结合模式。

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