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胸腺细胞抗原不会在CD4+ T细胞区室中诱导耐受性。

Thymocyte antigens do not induce tolerance in the CD4+ T cell compartment.

作者信息

Jhaver K G, Chandler P, Simpson E, Mellor A L

机构信息

Program in Molecular Immunology, Institute of Molecular Medicine and Genetics, Medical College of Georgia, Augusta 30912, USA.

出版信息

J Immunol. 1999 Nov 1;163(9):4851-8.

Abstract

Thymocytes fail to tolerize the developing T cell repertoire to self MHC class I (MHC I) Ags because transgenic (CD2Kb) mice expressing H-2Kb solely in lymphoid cell lineages reject skin grafts mismatched only for H-2Kb. In this study, we examined why thymocytes fail to tolerize the T cell repertoire to self MHC I Ags. The ability of CD2Kb mice to reject H-2Kb skin grafts was age dependent because CD2Kb mice older than 20 wk accepted skin grafts. T cells from younger CD2Kb mice proliferated, but did not develop cytotoxic functions in vitro in response to H-2Kb. Proliferative responses were dominated by H-2Kb-specific, CD4+ T cells rather than CD8+ T cells. Representative CD4+ T cell clones from CD2Kb mice were MHC II restricted and recognized processed H-2Kb. TCR transgenic mice were generated from one CD4+ T cell clone (361) to monitor development of H-2Kb-specific immature thymocytes when all thymic cells or lymphoid cell lineages only expressed H-2Kb. Thymocyte precursors were not eliminated and mice were not tolerant to H-2Kb when Tg361 TCR transgenic mice were intercrossed with CD2Kb mice. In contrast, all thymocyte precursors were eliminated efficiently in thymic microenvironments in which all cells expressed H-2Kb. We conclude that self MHC I Ags expressed exclusively in thymocytes do not induce T cell tolerance because presentation of processed self MHC I Ags on self MHC II molecules fails to induce negative selection of CD4+ T cell precursors. This suggests that some self Ags are effectively compartmentalized and cannot induce self-tolerance in the T cell repertoire.

摘要

胸腺细胞无法使发育中的T细胞库对自身MHC I类(MHC I)抗原产生耐受,因为仅在淋巴谱系细胞中表达H-2Kb的转基因(CD2Kb)小鼠会排斥仅在H-2Kb上不匹配的皮肤移植。在本研究中,我们探究了胸腺细胞无法使T细胞库对自身MHC I抗原产生耐受的原因。CD2Kb小鼠排斥H-2Kb皮肤移植的能力具有年龄依赖性,因为20周龄以上的CD2Kb小鼠会接受皮肤移植。来自年轻CD2Kb小鼠的T细胞会增殖,但在体外对H-2Kb无细胞毒性功能的发育。增殖反应以H-2Kb特异性的CD4⁺ T细胞而非CD8⁺ T细胞为主导。从CD2Kb小鼠中获得具有代表性的CD4⁺ T细胞克隆,这些克隆受MHC II限制并识别加工后的H-2Kb。当所有胸腺细胞或仅淋巴谱系细胞表达H-2Kb时,从一个CD4⁺ T细胞克隆(361)产生TCR转基因小鼠,以监测H-2Kb特异性未成熟胸腺细胞的发育。当Tg361 TCR转基因小鼠与CD2Kb小鼠杂交时,胸腺细胞前体未被清除,小鼠对H-2Kb也不耐受。相反在所有细胞均表达H-2Kb的胸腺微环境中,所有胸腺细胞前体被有效清除。我们得出结论,仅在胸腺细胞中表达的自身MHC I抗原不会诱导T细胞耐受,因为加工后的自身MHC I抗原在自身MHC II分子上的呈递未能诱导CD4⁺ T细胞前体的阴性选择。这表明一些自身抗原被有效地分隔开,无法在T细胞库中诱导自身耐受。

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