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细胞表面整合素亲和力的调控。

Regulation of integrin affinity on cell surfaces.

机构信息

Department of Pathology, Harvard Medical School, Immune Disease Institute and Children's Hospital, Boston, MA, USA.

出版信息

EMBO J. 2011 Sep 23;30(23):4712-27. doi: 10.1038/emboj.2011.333.

Abstract

Lymphocyte activation triggers adhesiveness of lymphocyte function-associated antigen-1 (LFA-1; integrin α(L)β(2)) for intercellular adhesion molecules (ICAMs) on endothelia or antigen-presenting cells. Whether the activation signal, after transmission through multiple domains to the ligand-binding αI domain, results in affinity changes for ligand has been hotly debated. Here, we present the first comprehensive measurements of LFA-1 affinities on T lymphocytes for ICAM-1 under a broad array of activating conditions. Only a modest increase in affinity for soluble ligand was detected after activation by chemokine or T-cell receptor ligation, conditions that primed LFA-1 and robustly induced lymphocyte adhesion to ICAM-1 substrates. By stabilizing well-defined LFA-1 conformations by Fab, we demonstrate the absolute requirement of the open LFA-1 headpiece for adhesiveness and high affinity. Interaction of primed LFA-1 with immobilized but not soluble ICAM-1 triggers energy-dependent affinity maturation of LFA-1 to an adhesive, high affinity state. Our results lend support to the traction or translational motion dependence of integrin activation.

摘要

淋巴细胞激活触发淋巴细胞功能相关抗原-1(LFA-1;整合素α(L)β(2))与内皮细胞或抗原呈递细胞上的细胞间黏附分子(ICAMs)的黏附性。激活信号在通过多个结构域传递到配体结合的αI 结构域后,是否会导致对配体的亲和力发生变化,这一直是激烈争论的话题。在这里,我们首次在广泛的激活条件下全面测量了 T 淋巴细胞上 LFA-1 对 ICAM-1 的亲和力。在用趋化因子或 T 细胞受体配体激活后,仅检测到对可溶性配体的亲和力适度增加,这些条件使 LFA-1 成熟,并强烈诱导淋巴细胞与 ICAM-1 底物的黏附。通过 Fab 稳定定义明确的 LFA-1 构象,我们证明了开放的 LFA-1 头部片段对于黏附性和高亲和力的绝对要求。与固定但不溶性的 ICAM-1 相互作用的成熟的 LFA-1 触发 LFA-1 向具有黏附性和高亲和力的激活状态的能量依赖性亲和力成熟。我们的结果支持整合素激活的牵引力或平移运动依赖性。

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Regulation of integrin affinity on cell surfaces.细胞表面整合素亲和力的调控。
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