A role for E2F1 in the induction of apoptosis during thymic negative selection.

I García, M Murga, A Vicario, S J Field, A M Zubiaga
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Abstract

Thymic negative selection is the process in which maturing thymocytes that express T-cell receptors recognizing self are eliminated by apoptotic cell death. The molecular mechanism by which this occurs is poorly understood. Notably, genes involved in cell death, even thymocyte death, such as Fas, Fas-ligand, p53, caspase-1, caspase-3, and caspase-9, and Bcl-2 have been found to not be required for normal thymic negative selection. We have demonstrated previously that E2F1-deficient mice have a defect in thymocyte apoptosis. Here we show that E2F1 is required for normal thymic negative selection. Furthermore, we observed an E2F1-dependent increase of p53 protein levels during the process of thymic clonal deletion, which suggests that E2F1 regulates activation-induced apoptosis of self-reactive thymocytes by a p53-dependent mechanism. In contrast, other apoptotic pathways operating on developing thymocytes, such as glucocorticoid-induced cell death, are not mediated by E2F1. The T lymphocytes that escape thymic negative selection migrate to the peripheral immune system but do not appear to be autoreactive, indicating that there may exist E2F1-independent mechanisms of peripheral tolerance, which protect mice from developing an autoimmune response. We expect that E2F1-deficient mice will provide a useful tool for understanding the molecular mechanism of and the immunological importance of thymic negative selection.

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胸腺阴性选择过程中E2F1在诱导细胞凋亡中的作用。
胸腺阴性选择是表达t细胞受体的成熟胸腺细胞因凋亡细胞死亡而被淘汰的过程。发生这种情况的分子机制尚不清楚。值得注意的是,参与细胞死亡甚至胸腺细胞死亡的基因,如Fas、Fas配体、p53、caspase-1、caspase-3、caspase-9和Bcl-2,已被发现在正常的胸腺阴性选择中并不需要。我们之前已经证明e2f1缺陷小鼠胸腺细胞凋亡有缺陷。这里我们发现E2F1是正常胸腺阴性选择所必需的。此外,在胸腺克隆缺失过程中,我们观察到E2F1依赖的p53蛋白水平升高,这表明E2F1通过p53依赖的机制调节激活诱导的自反应性胸腺细胞凋亡。相反,其他作用于发育中的胸腺细胞的凋亡途径,如糖皮质激素诱导的细胞死亡,不受E2F1介导。逃避胸腺阴性选择的T淋巴细胞迁移到外周免疫系统,但不表现出自身反应性,这表明可能存在不依赖于e2f1的外周耐受机制,保护小鼠免受自身免疫反应的影响。我们期望e2f1缺陷小鼠将为理解胸腺阴性选择的分子机制和免疫学重要性提供有用的工具。
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