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JAKs和STATs对T细胞稳态的调节。

Regulation of T cell homeostasis by JAKs and STATs.

作者信息

Ross Jeremy A, Nagy Zsuzsanna S, Cheng Hanyin, Stepkowski Stanislaw M, Kirken Robert A

机构信息

Department of Biological Sciences, University of Texas at El Paso, 500 W. University Ave., El Paso, TX, 79902, USA.

出版信息

Arch Immunol Ther Exp (Warsz). 2007 Jul-Aug;55(4):231-45. doi: 10.1007/s00005-007-0030-x. Epub 2007 Jul 23.

Abstract

Regulation of T cell homeostasis is critical for maintaining normal immune function. An imbalance in T cell proliferation can result in disorders ranging from cancer and autoimmunity to immunodeficiencies. Full activation of T cells requires three sequential signals, where signal 3, which is delivered by multiple cytokines, regulates proliferation, differentiation, and survival/death. Signaling from cytokines through their receptors is primarily delivered by two molecular families, namely Janus tyrosine kinases (JAKs) and signal transducers and activators of transcription (STATs). Invaluable knowledge about JAKs and STATs has arisen from studies of mice made genetically deficient in these molecules, analyses of tumor models, and studies of expression patterns by proteomics/genomics, which all have begun to define the role of JAKs and STATs in survival versus apoptosis. These findings also have suggested ways in which JAKs and STATs may be manipulated for therapeutic intervention in lymphoid-derived diseases. This review seeks to focus on the role of JAK tyrosine kinases and STAT transcription factors in mediating the lymphocyte life cycle and how they might be manipulated for therapeutic applications.

摘要

T细胞稳态的调节对于维持正常免疫功能至关重要。T细胞增殖失衡可导致从癌症、自身免疫到免疫缺陷等一系列疾病。T细胞的完全激活需要三个连续信号,其中由多种细胞因子传递的信号3调节增殖、分化和存活/死亡。细胞因子通过其受体发出的信号主要由两个分子家族传递,即Janus酪氨酸激酶(JAKs)和信号转导及转录激活因子(STATs)。关于JAKs和STATs的宝贵知识来自对这些分子基因缺陷小鼠的研究、肿瘤模型分析以及蛋白质组学/基因组学对表达模式的研究,所有这些研究都已开始确定JAKs和STATs在存活与凋亡中的作用。这些发现还提出了在淋巴源性疾病中操纵JAKs和STATs进行治疗干预的方法。本综述旨在聚焦JAK酪氨酸激酶和STAT转录因子在介导淋巴细胞生命周期中的作用,以及如何对其进行操纵以用于治疗应用。

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