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在CD4+8-T辅助淋巴细胞中诱导高水平白细胞介素-2的产生需要胸腺后发育。

Induction of high level IL-2 production in CD4+8- T helper lymphocytes requires post-thymic development.

作者信息

Chang J F, Thomas C A, Kung J T

机构信息

Department of Microbiology, University of Texas Health Science Center, San Antonio 78284.

出版信息

J Immunol. 1991 Aug 1;147(3):851-9.

PMID:1677670
Abstract

Triggering of the CD3:TCR complex by optimal concentrations of anti-CD3, anti-TCR beta-chain, and allogeneic stimulator cells induced dramatically higher levels (fivefold for anti-CD3, greater than 10-fold for anti-TCR beta-chain, 84-fold for alloantigen) of IL-2 production in spleen CD4+8- T cells than their thymic counterparts, despite comparable levels of CD3 and TCR beta-chain expression. The nature of the reduced IL-2 production was examined by analysis of anti-CD3-induced IL-2 production at the single cell level. The frequency of IL-2-producing cells in spleen CD4+8- T cells (40.0%) was approximately threefold that of thymus CD4+8- T cells (14.5%). Furthermore, the average IL-2 levels among positive IL-2 producers was also approximately threefold higher in spleen CD4+8- T cells than their thymic counterparts. Adoptive transfer of purified Thy-1.2+ CD4+8- T cells into Thy-1.1-congenic hosts provided a physiologic and histocompatible system that enabled identification of transferred donor (Thy-1.2+) among a sea of host (Thy-1.2-) CD4+ T cells, whose immune function with respect to IL-2 inducibility was examined after isolation by electronic cell sorting. Donor CD4+ T cells thus isolated from host spleen shortly (1 day) after i.v. transfer of thymus CD4+8- T cells were similar to freshly isolated thymus CD4+8- T cells in that they both produced little IL-2 in response to anti-CD3. However, by day 3 post-transfer, IL-2 production by donor CD4+8- T cells had more than doubled and by day 8, they produced IL-2 levels comparable to those of host spleen CD4+8- T cells. A similar acquisition of high level IL-2 inducibility in thymus CD4+8- T cells upon i.v. transfer into Thy-1.1-congenic hosts was also observed using allogeneic cells as the stimulus of IL-2 production. When thymus CD4+8- T cells were intra-thymically transferred into Thy-1.1-congenic hosts, those donor cells that emigrated to the periphery became high IL-2 producers in a time-dependent manner, whereas those that remained inside the thymus showed no signs of up-regulation in IL-2 inducibility. Intrathymic transfer of CD4-8- thymocytes revealed that the most recent thymic emigrant CD4+8- T cells contained few IL-2-producing cells and were not functionally mature with respect to high level IL-2 inducibility.

摘要

用最佳浓度的抗CD3、抗TCRβ链和同种异体刺激细胞触发CD3:TCR复合物,在脾脏CD4+8-T细胞中诱导产生的白细胞介素-2(IL-2)水平比胸腺中的对应细胞显著更高(抗CD3诱导的为五倍,抗TCRβ链诱导的大于10倍,同种异体抗原诱导的为84倍),尽管CD3和TCRβ链的表达水平相当。通过在单细胞水平分析抗CD3诱导的IL-2产生,研究了IL-2产生减少的本质。脾脏CD4+8-T细胞中产生IL-2的细胞频率(40.0%)约为胸腺CD4+8-T细胞(14.5%)的三倍。此外,脾脏CD4+8-T细胞中IL-2阳性产生者的平均IL-2水平也比胸腺中的对应细胞高出约三倍。将纯化的Thy-1.2+CD4+8-T细胞过继转移到Thy-1.1同基因宿主中,提供了一个生理和组织相容性系统,能够在宿主(Thy-1.2-)CD4+T细胞的海洋中识别转移的供体(Thy-1.2+)细胞,通过电子细胞分选分离后,检测其关于IL-2诱导性的免疫功能。静脉注射胸腺CD4+8-T细胞后不久(1天)从宿主脾脏中分离出的供体CD4+T细胞,与新鲜分离的胸腺CD4+8-T细胞相似,即它们对抗CD3刺激均产生很少的IL-2。然而,转移后第3天,供体CD4+8-T细胞的IL-2产生增加了一倍多,到第8天,它们产生的IL-2水平与宿主脾脏CD4+8-T细胞相当。使用同种异体细胞作为IL-2产生的刺激物,静脉注射到Thy-1.1同基因宿主中时,胸腺CD4+8-T细胞也观察到类似的高水平IL-2诱导性的获得。当胸腺CD4+8-T细胞胸腺内转移到Thy-1.1同基因宿主中时,那些迁移到外周的供体细胞以时间依赖性方式成为高IL-2产生者,而那些留在胸腺内的细胞没有显示出IL-2诱导性上调的迹象。CD4-8-胸腺细胞的胸腺内转移显示,最新迁出胸腺的CD4+8-T细胞中产生IL-2的细胞很少,并且在高水平IL-2诱导性方面功能不成熟。

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