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Structural basis of activation-dependent binding of ligand-mimetic antibody AL-57 to integrin LFA-1

机译:配体模拟抗体AL-57与整联蛋白LFA-1活化依赖性结合的结构基础

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摘要

The activity of integrin LFA-1 (αLβ2) to its ligand ICAM-1 is regulated through the conformational changes of its ligand-binding domain, the I domain of αL chain, from an inactive, low-affinity closed form (LA), to an intermediate-affinity form (IA), and then finally, to a high-affinity open form (HA). A ligand-mimetic human monoclonal antibody AL-57 (activated LFA-1 clone 57) was identified by phage display to specifically recognize the affinity-upregulated I domain. Here, we describe the crystal structures of the Fab fragment of AL-57 in complex with IA, as well as in its unligated form. We discuss the structural features conferring AL-57's strong selectivity for the high affinity, open conformation of the I domain. The AL-57-binding site overlaps the ICAM-1 binding site on the I domain. Furthermore, an antibody Asp mimics an ICAM Glu by forming a coordination to the metal-ion dependent adhesion site (MIDAS). The structure also reveals better shape complementarity and a more hydrophobic interacting interface in AL-57 binding than in ICAM-1 binding. The results explain AL-57's antagonistic mimicry of LFA-1's natural ligands, the ICAM molecules.
机译:整联蛋白LFA-1(αLβ2)对其配体ICAM-1的活性通过其配体结合结构域(αL链的I结构域)从无活性,低亲和力封闭形式(LA)到中间亲和形式(IA),最后是高亲和开放形式(HA)。通过噬菌体展示鉴定出模拟配体的人单克隆抗体AL-57(活化的LFA-1克隆57),以特异性识别亲和力上调的I结构域。在这里,我们描述了与IA复合的AL-57 Fab片段的晶体结构,以及其未连接形式。我们讨论赋予AL-57对I结构域高亲和力,开放构象的强选择性的结构特征。 AL-57结合位点在I结构域上与ICAM-1结合位点重叠。此外,抗体Asp通过与金属离子依赖性粘附位点(MIDAS)形成配位来模拟ICAM Glu。该结构还显示出比ICAM-1结合更好的形状互补性和AL-57结合更好的疏水相互作用界面。结果解释了AL-57对LFA-1天然配体ICAM分子的拮抗模拟作用。

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