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整合素信号转导中跨膜结构域相互作用的结构基础。

Structural basis of transmembrane domain interactions in integrin signaling.

机构信息

Department of Biochemistry & Molecular Biology and Zilkha Neurogenetic Institute, Keck School of Medicine, University of Southern California, Los Angeles, CA, USA.

出版信息

Cell Adh Migr. 2010 Apr-Jun;4(2):243-8. doi: 10.4161/cam.4.2.10592. Epub 2010 Apr 10.

Abstract

Cell surface receptors of the integrin family are pivotal to cell adhesion and migration. The activation state of heterodimeric alphabeta integrins is correlated to the association state of the single-pass alpha and beta transmembrane domains. The association of integrin alphaIIbbeta3 transmembrane domains, resulting in an inactive receptor, is characterized by the asymmetric arrangement of a straight (alphaIIb) and tilted (beta3) helix relative to the membrane in congruence to the dissociated structures. This allows for a continuous association interface centered on helix-helix glycine-packing and an unusual alphaIIb(GFF) structural motif that packs the conserved Phe-Phe residues against the beta3 transmembrane helix, enabling alphaIIb(D723)beta3(R995) electrostatic interactions. The transmembrane complex is further stabilized by the inactive ectodomain, thereby coupling its association state to the ectodomain conformation. In combination with recently determined structures of an inactive integrin ectodomain and an activating talin/beta complex that overlap with the alphabeta transmembrane complex, a comprehensive picture of integrin bi-directional transmembrane signaling has emerged.

摘要

细胞表面整联蛋白家族的受体对于细胞黏附和迁移至关重要。异二聚体 αβ 整联蛋白的激活状态与单次跨膜结构域的 α 和 β 亚基的缔合状态相关。整联蛋白 αIIbbeta3 跨膜结构域的缔合导致无活性受体,其特征是相对于膜的直(αIIb)和倾斜(β3)螺旋的不对称排列与分离结构一致。这允许以螺旋-螺旋甘氨酸包装为中心的连续缔合界面和不寻常的 αIIb(GFF)结构基序,该基序将保守的 Phe-Phe 残基包装在β3 跨膜螺旋上,从而实现 αIIb(D723)β3(R995)静电相互作用。非活性胞外结构域进一步稳定了跨膜复合物,从而将其缔合状态与胞外结构域构象偶联。结合最近确定的无活性整联蛋白胞外结构域和与 αβ 跨膜复合物重叠的激活 talin/β 复合物的结构,整联蛋白双向跨膜信号传递的全貌已经浮现。

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