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早期生长反应转录因子与免疫应答的调节:对自身免疫的影响。

Early growth response transcription factors and the modulation of immune response: implications towards autoimmunity.

机构信息

Department of Immunology and Rheumatology, Instituto Nacional de Ciencias Médicas y Nutrición Salvador Zubirán, Vasco de Quiroga 15, Tlalpan 14000, Mexico City, Mexico.

出版信息

Autoimmun Rev. 2010 Apr;9(6):454-8. doi: 10.1016/j.autrev.2009.12.006. Epub 2009 Dec 23.

Abstract

Early Growth Response (EGR) zinc finger transcription factors are induced under diverse mitogenic signals on different cell types such as lymphocytes. Their genetic expression does not require de novo protein synthesis, which suggests its role as immediate response mediators between cell surface receptor signaling and gene expression regulation. EGR factors are involved in modulating the immune response, by means of the induction of differentiation of lymphocyte precursors, activation of T and B cells, as well as their involvement in central and peripheral tolerance. The maturation state, particularly for B cells, and signaling through the T or B cell receptors seems to be quite relevant for the induction of the expression of these transcription factors. EGR-1 functions as a positive regulatory factor for B and T cells mediated by transcriptional regulation of key cytokines and costimulatory molecules, and its interaction with NFAT. On the opposite, EGR-2 and 3 act as negative regulators involved in anergy induction and apoptosis. EGR-2 and 3 deficiency has been related to the development of lupus like disease in murine models. The deficiency of these transcription factors has been associated to deficient Cbl-b expression, a resistant to anergy phenotype, and expansion of effector and activated T cells.

摘要

早期生长反应 (EGR) 锌指转录因子在不同的有丝分裂信号下诱导,在不同的细胞类型中,如淋巴细胞。它们的基因表达不需要新的蛋白质合成,这表明它们作为细胞表面受体信号和基因表达调控之间的即时反应介质的作用。EGR 因子通过诱导淋巴细胞前体的分化、T 和 B 细胞的激活,以及它们在中枢和外周耐受中的参与,参与调节免疫反应。成熟状态,特别是对于 B 细胞,以及通过 T 或 B 细胞受体的信号传导,似乎与这些转录因子表达的诱导相当相关。EGR-1 通过关键细胞因子和共刺激分子的转录调节,作为 B 和 T 细胞的正向调节因子起作用,并且与 NFAT 相互作用。相反,EGR-2 和 3 作为涉及失能诱导和细胞凋亡的负调节因子起作用。在鼠模型中,EGR-2 和 3 的缺失与狼疮样疾病的发展有关。这些转录因子的缺失与 Cbl-b 表达不足、对失能的抗性表型以及效应器和激活 T 细胞的扩增有关。

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