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C反应蛋白与淋巴细胞和单核细胞的相互作用:补体依赖性黏附和吞噬作用。

Interaction of C-reactive protein with lymphocytes and monocytes: complement-dependent adherence and phagocytosis.

作者信息

Mortensen R F, Osmand A P, Lint T F, Gewurz H

出版信息

J Immunol. 1976 Sep;117(3):774-81.

PMID:60448
Abstract

The serum constituent C-reactive protein (CRP), which activates the classical complement (C) pathway when reacting with its substrates, was examined for its ability to mediate reactions of opsonic adherence and phagocytosis. Erythrocytes coated with C-polysaccharide (CPS) and reacted with CRP (E. CPS-CRP) failed to adhere to B cells and displayed only minimal adherence to monocytes. However, upon the addition of absorbed C or purified C components these cells were found to possess the cleavage products C4b and C3b, which in turn resulted in attachment of these cells to both human B lymphocytes and peripheral blood monocytes. E. CPS-CRP treated with C in the absence of antibody were readily phagocytosized by glass-adherent human monocytes. The phagocytosis of E. CPS-CRP-C was not only mediated by CRP but also required the presence of CRP on the surface of the red cells. The extent of ingestion was proportional to the amount of CRP on the red cell intermediate and was reduced by blocking monocyte receptors with aggregated human gamma-globulin (HGG) at concentrations which did not impair the uptake of other particles. The mediation by CRP of reactions of opsonic adherence and phagocytosis as outlined in these studies points to a significant role for CRP in reactions of host defense and inflammation.

摘要

血清成分C反应蛋白(CRP)在与其底物反应时会激活经典补体(C)途径,我们检测了其介导调理吞噬黏附反应和吞噬作用的能力。用C多糖(CPS)包被并与CRP反应的红细胞(E.CPS-CRP)无法黏附于B细胞,对单核细胞的黏附也很微弱。然而,加入吸收的C或纯化的C成分后,发现这些细胞具有裂解产物C4b和C3b,这进而导致这些细胞黏附于人类B淋巴细胞和外周血单核细胞。在无抗体情况下用C处理的E.CPS-CRP很容易被玻璃黏附的人类单核细胞吞噬。E.CPS-CRP-C的吞噬作用不仅由CRP介导,还需要红细胞表面存在CRP。摄取程度与红细胞中间体上CRP的量成正比,并且通过用聚集的人γ球蛋白(HGG)阻断单核细胞受体来降低摄取程度,所用浓度不会损害其他颗粒的摄取。这些研究中概述的CRP对调理吞噬黏附反应和吞噬作用的介导表明CRP在宿主防御和炎症反应中具有重要作用。

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