Department of Biological Chemistry and Molecular Pharmacology, Immune Disease Institute and Children's Hospital, Boston, MA 02115, USA.
J Cell Biol. 2012 Jan 9;196(1):131-46. doi: 10.1083/jcb.201110023.
The lymphocyte homing receptor integrin α(4)β(7) is unusual for its ability to mediate both rolling and firm adhesion. α(4)β(1) and α(4)β(7) are targeted by therapeutics approved for multiple sclerosis and Crohn's disease. Here, we show by electron microscopy and crystallography how two therapeutic Fabs, a small molecule (RO0505376), and mucosal adhesion molecule-1 (MAdCAM-1) bind α(4)β(7). A long binding groove at the α(4)-β(7) interface for immunoglobulin superfamily domains differs in shape from integrin pockets that bind Arg-Gly-Asp motifs. RO0505376 mimics an Ile/Leu-Asp motif in α(4) ligands, and orients differently from Arg-Gly-Asp mimics. A novel auxiliary residue at the metal ion-dependent adhesion site in α(4)β(7) is essential for binding to MAdCAM-1 in Mg(2+) yet swings away when RO0505376 binds. A novel intermediate conformation of the α(4)β(7) headpiece binds MAdCAM-1 and supports rolling adhesion. Lack of induction of the open headpiece conformation by ligand binding enables rolling adhesion to persist until integrin activation is signaled.
淋巴细胞归巢受体整合素 α(4)β(7) 因其能够介导滚动和牢固黏附的能力而不同寻常。α(4)β(1) 和 α(4)β(7) 是已被批准用于多发性硬化症和克罗恩病的治疗药物的靶点。在这里,我们通过电子显微镜和晶体学显示了两种治疗性 Fab、一种小分子(RO0505376)和黏膜黏附分子-1(MAdCAM-1)如何与 α(4)β(7)结合。在 α(4)-β(7) 界面处的免疫球蛋白超家族结构域的长结合槽的形状与结合 Arg-Gly-Asp 基序的整合素口袋不同。RO0505376 模拟 α(4)配体中的 Ile/Leu-Asp 基序,与 Arg-Gly-Asp 模拟物的取向不同。在 α(4)β(7) 的金属离子依赖性黏附位点的一个新的辅助残基对于在 Mg2+中与 MAdCAM-1 的结合是必需的,但当 RO0505376 结合时,它会摆动离开。α(4)β(7) 头部的一个新的中间构象结合 MAdCAM-1 并支持滚动黏附。配体结合时没有诱导开放头部构象的形成,从而使滚动黏附能够持续存在,直到整合素被激活。
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