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吞噬细胞上的黏附促进受体。

Adhesion-promoting receptors on phagocytes.

作者信息

Wright S D, Detmers P A

机构信息

Laboratory of Cellular Physiology and Immunology, Rockefeller University, New York, NY 10021.

出版信息

J Cell Sci Suppl. 1988;9:99-120. doi: 10.1242/jcs.1988.supplement_9.5.

Abstract

Phagocytes express a family of structurally related receptors, LFA-1, CR3, and p150,95, that mediate adhesion of leukocytes to a variety of cells and surfaces. LFA-1 mediates the binding of killer T cells to targets, CR3 mediates binding of phagocytes to iC3b-coated surfaces and to endothelial cells, and LFA-1, CR3, and p150,95 each mediate the binding of bacterial lipopolysaccharide. Here we review the structure and function of each of these receptors and present evidence that they are related to a larger class of adhesion-promoting receptors called integrins. Of particular emphasis are observations that the capacity of these receptors to promote adhesion is strongly and reversibly modulated by both soluble and surface-bound stimuli. We review this form of regulation and present evidence that changes in the binding activity of adhesion-promoting receptors is accomplished by changes in the two-dimensional distribution of receptors in the plane of the membrane. Inactive receptors are randomly distributed in the membrane, and their ability to bind a ligand-coated surface is enabled by a ligand-independent movement into small clusters. The implications of these structural features are discussed.

摘要

吞噬细胞表达一族结构相关的受体,即淋巴细胞功能相关抗原-1(LFA-1)、补体受体3(CR3)和p150,95,它们介导白细胞与多种细胞及表面的黏附。LFA-1介导杀伤性T细胞与靶标的结合,CR3介导吞噬细胞与iC3b包被的表面及内皮细胞的结合,并且LFA-1、CR3和p150,95均介导细菌脂多糖的结合。在此,我们综述这些受体各自的结构与功能,并提供证据表明它们与一类更大的促进黏附的受体家族即整合素相关。特别值得强调的是,这些受体促进黏附的能力受到可溶性刺激和表面结合刺激的强烈且可逆的调节。我们综述这种调节形式,并提供证据表明促进黏附的受体结合活性的变化是通过膜平面中受体二维分布的改变来实现的。无活性的受体随机分布于膜中,它们结合配体包被表面的能力通过不依赖配体的移动形成小簇而得以实现。我们讨论了这些结构特征的意义。

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