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细胞外钙会导致中性粒细胞上的Mac-1(CD11b/CD18)发生构象变化。Mac-1的黏附与吞噬功能分化。

Extracellular calcium results in a conformational change in Mac-1 (CD11b/CD18) on neutrophils. Differentiation of adhesion and phagocytosis functions of Mac-1.

作者信息

Graham I L, Brown E J

机构信息

Department of Medicine, Washington University Medical School, St. Louis, MO 63110.

出版信息

J Immunol. 1991 Jan 15;146(2):685-91.

PMID:1702813
Abstract

Mac-1 is a leukocyte integrin involved in multiple adhesion phenomena and also in the phagocytosis of particles that are bound via CR1 and the IgG FcR. We examined the divalent cation requirements for the Mac-1-dependent processes of adhesion and receptor-mediated phagocytosis. With phorbol ester stimulation, both processes occurred in the absence of extracellular Ca+2. In Ca+2-containing buffer, IB4, an anti-beta 2 mAb, inhibited both adhesion and CR1-mediated ingestion. In the absence of Ca+2, IB4 no longer had any effect on ingestion, although it continued to inhibit adhesion to protein-coated plastic completely. This demonstrates that the role of Mac-1 in adhesion is distinct from its role in phagocytosis. In addition, 1) IB4 did not change intracellular Ca+2 homeostasis; 2) as little as 300 nM free extracellular Ca+2 could restore the ability of IB4 to inhibit ingestion; and 3) in the absence of extracellular Ca+2, Mac-1 was more susceptible to enzymatic cleavage. Together these data suggest a Ca+2-dependent conformational change in Mac-1, which allows distinction of the roles of Mac-1 in phagocytosis and adhesion.

摘要

Mac-1是一种白细胞整合素,参与多种黏附现象以及通过CR1和IgG FcR结合的颗粒的吞噬作用。我们研究了Mac-1依赖性黏附过程和受体介导的吞噬作用对二价阳离子的需求。在佛波酯刺激下,这两个过程在没有细胞外Ca+2的情况下发生。在含Ca+2的缓冲液中,抗β2单克隆抗体IB4抑制黏附和CR1介导的摄取。在没有Ca+2的情况下,IB4对摄取不再有任何影响,尽管它继续完全抑制对蛋白包被塑料的黏附。这表明Mac-1在黏附中的作用与其在吞噬作用中的作用不同。此外,1)IB4不改变细胞内Ca+2稳态;2)低至300 nM的游离细胞外Ca+2可恢复IB4抑制摄取的能力;3)在没有细胞外Ca+2的情况下,Mac-1更容易受到酶解作用。这些数据共同表明Mac-1中存在Ca+2依赖性构象变化,这使得能够区分Mac-1在吞噬作用和黏附中的作用。

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