首页> 美国卫生研究院文献>Infection and Immunity >Identification of the leukocyte adhesion molecules CD11 and CD18 as receptors for type 1-fimbriated (mannose-specific) Escherichia coli.
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Identification of the leukocyte adhesion molecules CD11 and CD18 as receptors for type 1-fimbriated (mannose-specific) Escherichia coli.

机译:识别白细胞粘附分子CD11和CD18作为1型纤维化(甘露糖特异性)大肠杆菌的受体。

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摘要

Attachment of bacteria to phagocytic cells may be mediated by lectin-carbohydrate interactions, resulting in lectinophagocytosis. The best-studied system is the interaction of type 1-fimbriated (mannose-specific) Escherichia coli with human phagocytic cells. Here we demonstrate that the leukocyte integrins CD11 and CD18 (CD11/CD18) constitute the major receptors for type 1-fimbriated E. coli. Bacteria were bound in a dose-dependent and saturable manner to CD11/CD18, which was immobilized to microwells, whereas nonfimbriated E. coli cells failed to bind. The binding was efficiently inhibited (82 to 85%) by methyl-alpha-mannoside but not by galactose, and it was reduced by treatment of the immobilized CD11/CD18 with sodium metaperiodate, endoglycosidase H, or a mixture of endoglycosidase F and N-glycosidase. The fimbriated bacteria also bound to CD11a,b,c and CD18 separated by polyacrylamide gel electrophoresis with sodium dodecyl sulfate and blotted onto nitrocellulose paper. This binding was inhibited specifically by methyl-alpha-mannoside and was significantly diminished by treatment of the blots with sodium metaperiodate. Only minimal binding to the blotted CD11/CD18 that had been deglycosylated enzymatically prior to electrophoresis was observed. On blots of granulocyte lysates, specific binding to two glycoproteins (Mrs, 90,000 to 100,000 and 165,000) with mobilities similar to that of CD11/CD18 was observed. Monoclonal antibodies to CD11a, CD11b, or CD18 inhibited the binding of the bacteria to intact human granulocytes by 55 to 80%, whereas antibodies against other leukocyte surface antigens were not inhibitory. We conclude that type 1-fimbriated E. coli binds to human granulocytes via the oligomannose and hybrid N-linked units of CD11/CD18. Since CD11b/CD18 and CD11c/CD18 are known to serve as receptors for complement fragment iC3b, this study provides a link between opsonophagocytosis and lectinophagocytosis.
机译:凝集素-碳水化合物相互作用可能介导细菌与吞噬细胞的附着,从而导致凝集素吞噬作用。研究最好的系统是1型纤维化(甘露糖特异性)大肠杆菌与人类吞噬细胞的相互作用。在这里,我们证明白细胞整合素CD11和CD18(CD11 / CD18)构成1型成纤维大肠杆菌的主要受体。细菌以剂量依赖性和饱和方式与固定在微孔上的CD11 / CD18结合,而未成膜的大肠杆菌细胞则无法结合。甲基-α-甘露糖苷可有效抑制结合(82%至85%),但半乳糖不会抑制结合,通过用过高碘酸钠,内切糖苷酶H或内切糖苷酶F和N-的混合物处理固定的CD11 / CD18可以减少结合。糖苷酶。滤过的细菌还与CD11a,b,c和CD18结合,用十二烷基硫酸钠通过聚丙烯酰胺凝胶电泳分离,并吸到硝酸纤维素纸上。这种结合被甲基-α-甘露糖苷特异性地抑制,并且通过用偏高碘酸钠处理印迹而显着降低了该结合。观察到与电泳前已被糖基化的脱墨CD11 / CD18的结合极少。在粒细胞裂解物的印迹上,观察到与两种糖蛋白(Mrs,90,000至100,000和165,000)的特异性结合,其迁移率与CD11 / CD18相似。针对CD11a,CD11b或CD18的单克隆抗体可将细菌与完整的人类粒细胞的结合抑制55%至80%,而针对其他白细胞表面抗原的抗体则不受抑制。我们得出的结论是,类型为1的大肠杆菌通过CD11 / CD18的低聚甘露糖和杂合N链单元与人粒细胞结合。由于已知CD11b / CD18和CD11c / CD18可以作为补体片段iC3b的受体,因此这项研究提供了调理吞噬作用和吞噬吞噬作用之间的联系。

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