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CD14的膜结合形式和可溶性形式均能与革兰氏阴性菌结合。

Both membrane-bound and soluble forms of CD14 bind to gram-negative bacteria.

作者信息

Jack R S, Grunwald U, Stelter F, Workalemahu G, Schütt C

机构信息

Institut für Immunologie und Transfusionsmedizin, Klinikum, Ernst-Moritz-Arndt-Universität, Greifswald, Germany.

出版信息

Eur J Immunol. 1995 May;25(5):1436-41. doi: 10.1002/eji.1830250545.

Abstract

Tissue macrophages and their precursors-the blood monocytes-respond rapidly to a bacterial infection with the release of inflammatory mediators. These mediators are involved in the recruitment of phagocytic cells, principally neutrophils, from the blood to the site of infection. To initiate this process macrophages and monocytes must be able to detect the presence of bacteria in a reliable, but nevertheless nonspecific, fashion. It is thought that this is achieved by means of receptors on the cell surface which recognize structures common to many different bacteria. One candidate for such a "pattern recognition element" is the cell surface glycoprotein CD14. CD14 has been shown to bind components of the Gram-positive cell wall and it also binds soluble lipopolysaccharide released from Gram-negative bacteria. In both cases the interaction with CD14 leads to an activation of the cell. Here we show that human peripheral blood monocytes can, in addition, bind intact Gram-negative bacteria in the presence of serum and this process involves CD14. When CD14 expression is induced on the myelomonocytic cell line U937 by treatment with vitamin D3 the cells concomittently acquire the capacity to bind bacteria. Furthermore, a non-monocytic cell line which does not bind bacteria acquires the capacity to do so when transfected with either the human or mouse CD14 gene. This binding can be inhibited by blocking the CD14 receptor with anti-CD14 antibody or by blocking the ligand on the bacteria with soluble CD14. Finally we demonstrate binding of sCD14 to Escherichia coli. We conclude that in the presence of serum both membrane-bound and soluble forms of CD14 can bind to Gram-negative bacteria. This suggests that CD14 may play a role in the detection and elimination of intact bacteria in vivo.

摘要

组织巨噬细胞及其前体——血液单核细胞,会通过释放炎症介质对细菌感染迅速做出反应。这些介质参与了吞噬细胞(主要是中性粒细胞)从血液到感染部位的募集过程。为启动这一过程,巨噬细胞和单核细胞必须能够以一种可靠但非特异性的方式检测到细菌的存在。据认为,这是通过细胞表面的受体来实现的,这些受体能够识别许多不同细菌共有的结构。这种“模式识别元件”的一个候选者是细胞表面糖蛋白CD14。已表明CD14能结合革兰氏阳性菌细胞壁的成分,它也能结合从革兰氏阴性菌释放的可溶性脂多糖。在这两种情况下,与CD14的相互作用都会导致细胞活化。在此我们表明,人类外周血单核细胞在有血清存在时还能结合完整的革兰氏阴性菌,且这一过程涉及CD14。当用维生素D3处理髓单核细胞系U937诱导其表达CD14时,细胞同时获得了结合细菌的能力。此外,一个不结合细菌的非单核细胞系在转染人或小鼠CD14基因后获得了这样做的能力。这种结合可以通过用抗CD14抗体阻断CD14受体或用可溶性CD14阻断细菌上的配体来抑制。最后我们证明了可溶性CD14与大肠杆菌的结合。我们得出结论,在有血清存在时,膜结合形式和可溶性形式的CD14都能与革兰氏阴性菌结合。这表明CD14可能在体内检测和清除完整细菌中发挥作用。

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