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激活后,人自然杀伤细胞上的CD11b和CD11c抗原会迅速增加。

CD11b and CD11c antigens are rapidly increased on human natural killer cells upon activation.

作者信息

Werfel T, Witter W, Götze O

机构信息

Department of Immunology, University of Göttingen, Federal Republic of Germany.

出版信息

J Immunol. 1991 Oct 1;147(7):2423-7.

PMID:1680915
Abstract

A brief incubation with PMA or other secretagogues has been reported to enhance the expression of C3 receptors on myeloid cells. We now observed increases up to threefold in the expression of the CD11b/CD18 Ag (CR3) and the CD11c/CD18 (CR4, p150,95) Ag after 30-min incubation with PMA on a subpopulation of PBL. The majority of these cells was CD56+ and CD16+. Isolated NK cells retained their ability to respond to PMA with increased CD11b and CD11c membrane Ag expression. Preincubation of the cells with cycloheximide did not abrogate the effects of PMA. Other membrane molecules on lymphocytes (CD11a, CD35, CD45, CD45R0, CD56) were not modulated by PMA. Purified C5a, FMLP, or LPS increased CR3 on myeloid cells but not on lymphocytes. In contrast, cell activation by K562 cells led to an augmentation of the CD11b Ag expression on CD56+ lymphocytes but not on other lymphocytes or monocytes. This increase was inhibitable by CD11a mAb. Rapid increases of CD11b and CD11c Ag on the membrane of NK cells may be of biologic significance because many functions have been attributed to these molecules.

摘要

据报道,用佛波酯(PMA)或其他促分泌素短暂孵育可增强髓样细胞上C3受体的表达。我们现在观察到,在PBL亚群上用PMA孵育30分钟后,CD11b/CD18抗原(CR3)和CD11c/CD18(CR4,p150,95)抗原的表达增加了两倍。这些细胞大多数是CD56+和CD16+。分离的NK细胞保留了对PMA作出反应并增加CD11b和CD11c膜抗原表达的能力。用放线菌酮对细胞进行预孵育并没有消除PMA的作用。淋巴细胞上的其他膜分子(CD11a、CD35、CD45、CD45R0、CD56)未受PMA调节。纯化的C5a、FMLP或LPS可增加髓样细胞上的CR3,但不会增加淋巴细胞上的CR3。相反,K562细胞激活细胞会导致CD56+淋巴细胞上的CD11b抗原表达增加,但不会导致其他淋巴细胞或单核细胞上的CD11b抗原表达增加。这种增加可被CD11a单克隆抗体抑制。NK细胞膜上CD11b和CD11c抗原的快速增加可能具有生物学意义,因为许多功能都归因于这些分子。

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