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携带补体和Fc受体的淋巴细胞亚群的分离与功能分析。

Separation and functional analysis of subpopulations of lymphocytes bearing complement and Fc receptors.

作者信息

Parish C R

出版信息

Transplant Rev. 1975;25:98-120. doi: 10.1111/j.1600-065x.1975.tb00727.x.

Abstract

A highly versatile procedure is described in this review which can be used to separate and obtain in pure form subpopulations of lymphoid cells which express different cell surface structures. The method is based on the observation that when rosetting and non-rosetting leukocytes are centrifuged on a cushion of Isopaque/Ficoll, the rosetting leukocytes and red cells sink whereas the non-rosetting leukocytes float. Thus, any subpopulation of leukocytes can be separated providing they can be identified by rosetting. The earlier sections of this review describe the method, its efficiency of separation and its advantages compared with other fractionation procedures. Subsequent sections describe experiments in which the procedure was specifically applied to separating Fc receptor (Fc+) and complement receptor (CR+) lymphocytes. On the basis of these two receptors it was possible to subdivide T and B lymphocytes into distinct subpopulations. Four subclasses of B lymphocytes were identified in mouse spleen (Fc+CR+,Fc+CR-,Fc-CR+ and Fc-CR-) and two subclasses of T cells were also detected (Fc+ and Fc-). The functional relevance of these subpopulations of lymphocytes was examined. It was found that in all cases examined, antigens could successfully activate CR+ B cells to produce antibody. However, only polymeric antigens, whether T-dependent or T-independent, were capable of triggering CR- B cells to synthesize antibody. Furthermore, preliminary experiments suggest that Fc receptors are present on functional B cells and helper T cells but are not expressed on cytotoxic T cells. On the basis of these results it is proposed that complement receptors on B lymphocytes provide an additional binding site which stabilizes the union between the antigen-specific receptors and soluble antigen. In contrast, due to their multi-determinant nature, polymeric antigens can avidly bind to B cells without involvement of the complement receptors. The possibility of Fc receptors playing a similar role in stabilizing the interaction of antigen with specific receptors on lymphocytes, particularly on T helper cells, is also discussed.

摘要

本综述描述了一种用途广泛的方法,可用于分离并以纯形式获得表达不同细胞表面结构的淋巴细胞亚群。该方法基于这样的观察结果:当玫瑰花结形成细胞和非玫瑰花结形成白细胞在异泛影葡胺/聚蔗糖垫层上离心时,形成玫瑰花结的白细胞和红细胞会下沉,而非玫瑰花结形成白细胞则会漂浮。因此,只要白细胞亚群能够通过形成玫瑰花结来识别,就可以将其分离出来。本综述的前几部分描述了该方法、其分离效率以及与其他分级分离程序相比的优势。后续部分描述了将该程序专门应用于分离Fc受体(Fc+)和补体受体(CR+)淋巴细胞的实验。基于这两种受体,有可能将T淋巴细胞和B淋巴细胞细分为不同的亚群。在小鼠脾脏中鉴定出了四类B淋巴细胞亚群(Fc+CR+、Fc+CR-、Fc-CR+和Fc-CR-),还检测到了两类T细胞亚群(Fc+和Fc-)。对这些淋巴细胞亚群的功能相关性进行了研究。结果发现,在所研究的所有情况下,抗原都能成功激活CR+B细胞产生抗体。然而,只有聚合抗原,无论其为T细胞依赖性还是T细胞非依赖性,才能触发CR-B细胞合成抗体。此外,初步实验表明,Fc受体存在于功能性B细胞和辅助性T细胞上,但在细胞毒性T细胞上不表达。基于这些结果,有人提出B淋巴细胞上的补体受体提供了一个额外的结合位点,可稳定抗原特异性受体与可溶性抗原之间的结合。相比之下,由于其多决定簇性质,聚合抗原可以在不涉及补体受体的情况下与B细胞 avidly 结合。还讨论了Fc受体在稳定抗原与淋巴细胞特别是辅助性T细胞上的特异性受体相互作用中发挥类似作用的可能性。

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