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Two Functional States of the CD11b A-Domain: Correlations with Key Features of Two Mn2+-complexed Crystal Structures

机译:CD11b A域的两个功能状态:与两个Mn2 +复合晶体结构的关键特征的相关性

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摘要

In the presence of bound Mn2+, the three- dimensional structure of the ligand-binding A-domain from the integrin CR3 (CD11b/CD18) is shown to exist in the “open” conformation previously described only for a crystalline Mg2+ complex. The open conformation is distinguished from the “closed” form by the solvent exposure of F302, a direct T209–Mn2+ bond, and the presence of a glutamate side chain in the MIDAS site. Approximately 10% of wild-type CD11b A-domain is present in an “active” state (binds to activation-dependent ligands, e.g., iC3b and the mAb 7E3). In the isolated domain and in the holoreceptor, the percentage of the active form can be quantitatively increased or abolished in F302W and T209A mutants, respectively. The iC3b-binding site is located on the MIDAS face and includes conformationally sensitive residues that undergo significant shifts in the open versus closed structures. We suggest that stabilization of the open structure is independent of the nature of the metal ligand and that the open conformation may represent the physiologically active form.
机译:在存在结合的Mn 2 + 的情况下,整联蛋白CR3(CD11b / CD18)的配体结合A结构域的三维结构显示为存在上述“开放”构象仅适用于Mg 2 + 晶体。 F302的溶剂暴露,直接的T209–Mn 2 + 键以及MIDAS位点中存在谷氨酸侧链,从而使开放构象与“封闭”构型区分开。大约10%的野生型CD11b A结构域以“活性”状态存在(与激活依赖性配体结合,例如iC3b和mAb 7E3)。在分离的结构域和全受体中,活性形式的百分比可以分别在F302W和T209A突变体中定量增加或取消。 iC3b结合位点位于MIDAS面上,并且包括构象敏感的残基,这些残基在开放结构与封闭结构中发生显着变化。我们建议开放结构的稳定与金属配体的性质无关,并且开放构象可能代表生理活性形式。

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