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The αβ T Cell Receptor Is an Anisotropic Mechanosensor

机译:αβT细胞受体是各向异性的机械传感器

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摘要

Thymus-derived lymphocytes protect mammalian hosts against virus- or cancer-related cellular alterations through immune surveillance, eliminating diseased cells. In this process, T cell receptors (TCRs) mediate both recognition and T cell activation via their dimeric αβ, CD3ϵγ, CD3ϵδ, and CD3ζζ subunits using an unknown structural mechanism. Here, site-specific binding topology of anti-CD3 monoclonal antibodies (mAbs) and dynamic TCR quaternary change provide key clues. Agonist mAbs footprint to the membrane distal CD3ϵ lobe that they approach diagonally, adjacent to the lever-like Cβ FG loop that facilitates antigen (pMHC)-triggered activation. In contrast, a non-agonist mAb binds to the cleft between CD3ϵ and CD3γ in a perpendicular mode and is stimulatory only subsequent to an external tangential but not a normal force (∼50 piconewtons) applied via optical tweezers. Specific pMHC but not irrelevant pMHC activates a T cell upon application of a similar force. These findings suggest that the TCR is an anisotropic mechanosensor, converting mechanical energy into a biochemical signal upon specific pMHC ligation during immune surveillance. Activating anti-CD3 mAbs mimic this force via their intrinsic binding mode. A common TCR quaternary change rather than conformational alterations can better facilitate structural signal initiation, given the vast array of TCRs and their specific pMHC ligands.
机译:胸腺来源的淋巴细胞可通过免疫监视保护哺乳动物宿主,使其免受病毒或癌症相关的细胞改变,从而消除患病细胞。在这个过程中,T细胞受体(TCR)通过未知的结构机制,通过其二聚体αβ,CD3ϵγ,CD3ϵδ和CD3ζζ亚基介导识别和T细胞活化。在这里,抗CD3单克隆抗体(mAb)的位点特异性结合拓扑和动态TCR第四级变化提供了关键线索。激动剂mAb沿对角线靠近膜远端CD3β瓣的足迹,与促进抗原(pMHC)触发的激活的杠杆状CβFG环相邻。相反,非激动剂mAb以垂直方式结合在CD3 +和CD3γ之间的缝隙上,并且仅在通过光镊施加外切线但不施加法向力(约50皮欧顿)之后才具有刺激性。特定的pMHC但不相关的pMHC在施加相似的力时会激活T细胞。这些发现表明,TCR是一种各向异性的机械传感器,在免疫监视过程中,经过特定的pMHC连接,会将机械能转换为生化信号。激活的抗CD3 mAb通过其固有的结合模式模拟了这种作用力。鉴于存在大量的TCR及其特定的pMHC配体,常见的TCR四元变化而非构象变化可以更好地促进结构信号的启动。

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