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由CD45RB定义的大鼠CD4 + T细胞亚群的功能:CD45RB-细胞对回忆抗原的反应要强得多,而在存在外源性白细胞介素-2的情况下,两个亚群的多克隆激活细胞产生干扰素的效率相同。

Functions of rat CD4+ T cell subsets defined by CD45RB: CD45RB- cells have a much stronger response to recall antigens, whereas polyclonally activated cells of both subsets are equally efficient producers of IFN in the presence of exogenous IL-2.

作者信息

Ericsson P O, Lindén O, Dohlsten M, Sjögren H O, Hedlund G

机构信息

Department of Tumor Immunology, Wallenberg Laboratory, University of Lund, Sweden.

出版信息

Cell Immunol. 1991 Feb;132(2):391-9. doi: 10.1016/0008-8749(91)90036-b.

Abstract

CD4+45RB- rat T cells were shown to respond strongly to recall antigens and produce IFN and TNF after polyclonal activation. Compared to CD4+45RB- cells, CD4+45RB+ cells showed a very weak response to recall antigens but produced higher amounts of IFN and TNF after polyclonal activation. Addition of rIL-2 reduced the difference between the subsets with respect to the level of IFN produced at 48 and 72 hr after activation, but did not influence the level of TNF production. The CD4+45RB- cells clearly showed a faster response to polyclonal activation than that of CD4+45RB+ cells detected as an earlier IFN production and CD25 expression. The earlier IFN production by the CD45RB- population could not only be explained by their faster production of IL-2, since the difference persisted when rIL-2 was added to both populations at the beginning of culture. We conclude that the CD4+45RB- rat T cell population resemble the CD4+45RA-0+ human T cell subset with respect to a good responsiveness to recall antigen and efficient production of IFN. However, the CD4+45RB+ rat T cell subset functionally differs from the CD4+45RA+0- human T cell subset. We suggest that the CD4+45RB+ subset comprises a major CD4+45RA+B+0- and a minor CD4+4+45A-B+0+ T cell subpopulation, the latter possibly mediating a response to recall antigen and the production of IFN.

摘要

已表明,CD4+45RB-大鼠T细胞对回忆抗原反应强烈,多克隆激活后可产生干扰素(IFN)和肿瘤坏死因子(TNF)。与CD4+45RB-细胞相比,CD4+45RB+细胞对回忆抗原的反应非常微弱,但多克隆激活后产生的IFN和TNF量更高。添加重组白细胞介素-2(rIL-2)可减少激活后48小时和72小时两个亚群在IFN产生水平上的差异,但不影响TNF的产生水平。CD4+45RB-细胞对多克隆激活的反应明显比CD4+45RB+细胞快,表现为更早产生IFN和表达CD25。CD45RB-群体更早产生IFN,这不能仅用其更快产生IL-2来解释,因为在培养开始时向两个群体中都添加rIL-2时,差异仍然存在。我们得出结论,CD4+45RB-大鼠T细胞群体在对回忆抗原的良好反应性和高效产生IFN方面类似于CD4+45RA-0+人类T细胞亚群。然而,CD4+45RB+大鼠T细胞亚群在功能上与CD4+45RA+0-人类T细胞亚群不同。我们认为,CD4+45RB+亚群包括一个主要的CD4+45RA+B+0-和一个次要的CD4+4+45A-B+0+ T细胞亚群,后者可能介导对回忆抗原的反应和IFN的产生。

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