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环孢素A抑制αβTCR转基因小鼠的阳性选择并延迟阴性选择。

Cyclosporin A inhibits positive selection and delays negative selection in alpha beta TCR transgenic mice.

作者信息

Urdahl K B, Pardoll D M, Jenkins M K

机构信息

Department of Microbiology, University of Minnesota, Minneapolis 55455.

出版信息

J Immunol. 1994 Mar 15;152(6):2853-9.

PMID:8144886
Abstract

Cyclosporin A (CsA) is an immunosuppressive drug that inhibits TCR-mediated signal transduction. This drug has two major effects on developing alpha beta thymocytes in normal mice: it blocks the development of most mature CD4+8- and CD4-8+ thymocytes and inhibits the deletion of some but not all self-specific thymocytes. The latter effect may explain how CsA treatment can paradoxically induce autoimmunity in certain situations. Here we investigated the effects of CsA on thymocyte development in transgenic mice that express on most of their T cells an alpha beta TCR specific for male H-Y Ag bound to H-2 Db class I molecules, a model system in which positive and negative selection have been clearly defined. Positive selection occurs in female mice, resulting in the development of mature CD4-CD8+ T cells, whereas negative selection occurs in male mice, resulting in the deletion of self-reactive CD4+8+ thymocytes. CsA blocked positive selection, as evidenced by the finding that most of the cells present in the thymuses of CsA-treated female mice were functionally immature precursors that expressed heat-stable Ag. In male mice, CsA delayed but did not prevent the deletion of most CD4+8+ thymocytes. A few transgenic thymocytes, however, were not deleted and achieved the TCR+, CD4-8+ phenotype of positively selected cells. Therefore, for a small subset of thymocytes, CsA may convert a normally negatively selecting TCR signal to a positively selecting one.

摘要

环孢素A(CsA)是一种免疫抑制药物,可抑制TCR介导的信号转导。该药物对正常小鼠发育中的αβ胸腺细胞有两个主要影响:它阻断了大多数成熟CD4+8-和CD4-8+胸腺细胞的发育,并抑制了部分而非全部自身特异性胸腺细胞的清除。后一种作用可能解释了CsA治疗在某些情况下如何反常地诱发自身免疫。在此,我们研究了CsA对转基因小鼠胸腺细胞发育的影响,这些转基因小鼠的大多数T细胞表达与H-2 Db I类分子结合的针对雄性H-Y抗原的αβTCR,这是一个已明确界定阳性和阴性选择的模型系统。阳性选择发生在雌性小鼠中,导致成熟CD4-CD8+ T细胞的发育,而阴性选择发生在雄性小鼠中,导致自身反应性CD4+8+胸腺细胞的清除。CsA阻断了阳性选择,这一发现证明,经CsA处理的雌性小鼠胸腺中存在的大多数细胞是功能不成熟的前体细胞,它们表达热稳定抗原。在雄性小鼠中,CsA延迟但并未阻止大多数CD4+8+胸腺细胞的清除。然而,少数转基因胸腺细胞未被清除,并获得了阳性选择细胞的TCR+、CD4-8+表型。因此,对于一小部分胸腺细胞,CsA可能将正常的阴性选择TCR信号转变为阳性选择信号。

相似文献

1
Cyclosporin A inhibits positive selection and delays negative selection in alpha beta TCR transgenic mice.环孢素A抑制αβTCR转基因小鼠的阳性选择并延迟阴性选择。
J Immunol. 1994 Mar 15;152(6):2853-9.
2
Altered thymocyte development resulting from expressing a deleting ligand on selecting thymic epithelium.在选择的胸腺上皮细胞上表达缺失配体导致胸腺细胞发育改变。
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Development of CD4-CD8- alpha beta TCR+NK1.1+ T lymphocytes: thymic selection by self antigen.CD4-CD8-αβTCR+NK1.1+T淋巴细胞的发育:自身抗原介导的胸腺选择。
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Development of TCR-gamma delta CD4-CD8+ alpha alpha but not TCR-alpha beta CD4-CD8+ alpha alpha i-IEL is resistant to cyclosporin A.TCR-γδ CD4-CD8+αα而非TCR-αβ CD4-CD8+αα i-IEL的发育对环孢素A具有抗性。
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Deletion of antigen-specific immature thymocytes by dendritic cells requires LFA-1/ICAM interactions.树突状细胞对抗原特异性未成熟胸腺细胞的清除需要淋巴细胞功能相关抗原-1/细胞间黏附分子相互作用。
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Signal for T-cell differentiation to a CD4 cell lineage is delivered by CD4 transmembrane region and/or cytoplasmic tail.T细胞向CD4细胞谱系分化的信号由CD4跨膜区和/或胞质尾传递。
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