Baum L L, James K K, Glaviano R R, Gewurz H
J Exp Med. 1983 Jan 1;157(1):301-11. doi: 10.1084/jem.157.1.301.
Functional NK activity can be removed from human PBL and from phagocyte- and T cell-depleted LGL preparations by treatment with antisera specific for C-reactive protein (CRP) in the presence of complement (C). Pretreatment of NK effector cells with high concentrations of anti-CRP in the absence of C also depletes functional activity. These results indicate that CRP or an antigenically similar molecule is present on a population of NK effector cells. Fluorescent antibody studies in which biotin-avidin amplification was used confirm the presence of surface CRP (S-CRP) on a small percentage of nonphagocytic peripheral blood mononuclear cells. S-CRP readily caps off, which suggest that removal by capping obviates killing by this cell population. This indicates that S-CRP or a molecule that co-caps with S-CRP may be required for successful effector-target cell interaction. The addition of exogenous CRP or CRP-CPS complexes, however, does not alter NK responses. A subpopulation of lymphoid cells responsible for functional NK activity therefore appears to bear surface CRP.
通过在补体(C)存在的情况下用针对C反应蛋白(CRP)的抗血清处理,可以从人外周血淋巴细胞(PBL)以及从去除吞噬细胞和T细胞的大颗粒淋巴细胞(LGL)制剂中去除功能性自然杀伤(NK)活性。在没有补体C的情况下,用高浓度的抗CRP预处理NK效应细胞也会耗尽其功能活性。这些结果表明,CRP或抗原性相似的分子存在于一群NK效应细胞上。使用生物素-抗生物素蛋白放大的荧光抗体研究证实,在一小部分非吞噬性外周血单核细胞上存在表面CRP(S-CRP)。S-CRP很容易被封闭,这表明通过封闭去除S-CRP可避免该细胞群体的杀伤作用。这表明S-CRP或与S-CRP共封闭的分子可能是效应细胞与靶细胞成功相互作用所必需的。然而,添加外源性CRP或CRP-磷酸胆碱(CPS)复合物不会改变NK反应。因此,负责功能性NK活性的淋巴细胞亚群似乎带有表面CRP。