T 细胞前受体在胸腺细胞β选择过程中拓扑样地探测自身配体。
Pre-T cell receptors topologically sample self-ligands during thymocyte β-selection.
机构信息
Laboratory of Immunobiology, Dana-Farber Cancer Institute, Boston, MA, USA.
Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
出版信息
Science. 2021 Jan 8;371(6525):181-185. doi: 10.1126/science.abe0918. Epub 2020 Dec 17.
Abstract
Self-discrimination, a critical but ill-defined molecular process programmed during thymocyte development, requires myriad pre-T cell receptors (preTCRs) and αβTCRs. Using x-ray crystallography, we show how a preTCR applies the concave β-sheet surface of its single variable domain (Vβ) to "horizontally" grab the protruding MHC α2-helix. By contrast, αβTCRs purpose all six complementarity-determining region (CDR) loops of their paired VαVβ module to recognize peptides bound to major histocompatibility complex molecules (pMHCs) in "vertical" head-to-head binding. The preTCR topological fit ensures that CDR3β reaches the peptide's featured C-terminal segment for pMHC sampling, establishing the subsequent αβTCR canonical docking mode. "Horizontal" docking precludes germline CDR1β- and CDR2β-MHC binding to broaden β-chain repertoire diversification before αβTCR-mediated selection refinement. Thus, one subunit successively attunes the recognition logic of related multicomponent receptors.
摘要
自身歧视是胸腺细胞发育过程中编程的一个关键但定义不明确的分子过程,需要无数的前 T 细胞受体(preTCR)和 αβTCR。我们使用 X 射线晶体学展示了 preTCR 如何使用其单个可变结构域(Vβ)的凹面 β 片层表面“水平”抓取突出的 MHC α2 螺旋。相比之下,αβTCR 则将其配对的 VαVβ 模块的六个互补决定区(CDR)环全部用于“垂直”头对头结合来识别与主要组织相容性复合物分子(pMHC)结合的肽。preTCR 的拓扑拟合确保 CDR3β 到达肽的特征性 C 末端片段进行 pMHC 采样,从而建立后续的 αβTCR 规范对接模式。“水平”对接排除了原始的 CDR1β 和 CDR2β-MHC 结合,从而在 αβTCR 介导的选择细化之前扩大 β 链库多样化。因此,一个亚基依次调整相关多组分受体的识别逻辑。
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