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人类T细胞中STAT5A和STAT5B靶基因的鉴定。

Identification of STAT5A and STAT5B target genes in human T cells.

作者信息

Kanai Takahiro, Seki Scott, Jenks Jennifer A, Kohli Arunima, Kawli Trupti, Martin Dorrelyn Patacsil, Snyder Michael, Bacchetta Rosa, Nadeau Kari C

机构信息

Division of Immunology and Allergy, Department of Pediatrics, School of Medicine, Stanford University, Stanford, California, United States of America.

Department of Genetics, School of Medicine, Stanford University, Stanford, California, United States of America.

出版信息

PLoS One. 2014 Jan 30;9(1):e86790. doi: 10.1371/journal.pone.0086790. eCollection 2014.

Abstract

Signal transducer and activator of transcription (STAT) comprises a family of universal transcription factors that help cells sense and respond to environmental signals. STAT5 refers to two highly related proteins, STAT5A and STAT5B, with critical function: their complete deficiency is lethal in mice; in humans, STAT5B deficiency alone leads to endocrine and immunological problems, while STAT5A deficiency has not been reported. STAT5A and STAT5B show peptide sequence similarities greater than 90%, but subtle structural differences suggest possible non-redundant roles in gene regulation. However, these roles remain unclear in humans. We applied chromatin immunoprecipitation followed by DNA sequencing using human CD4(+) T cells to detect candidate genes regulated by STAT5A and/or STAT5B, and quantitative-PCR in STAT5A or STAT5B knock-down (KD) human CD4(+) T cells to validate the findings. Our data show STAT5A and STAT5B play redundant roles in cell proliferation and apoptosis via SGK1 interaction. Interestingly, we found a novel, unique role for STAT5A in binding to genes involved in neural development and function (NDRG1, DNAJC6, and SSH2), while STAT5B appears to play a distinct role in T cell development and function via DOCK8, SNX9, FOXP3 and IL2RA binding. Our results also suggest that one or more co-activators for STAT5A and/or STAT5B may play important roles in establishing different binding abilities and gene regulation behaviors. The new identification of these genes regulated by STAT5A and/or STAT5B has major implications for understanding the pathophysiology of cancer progression, neural disorders, and immune abnormalities.

摘要

信号转导子和转录激活子(STAT)是一类通用转录因子家族,可帮助细胞感知并响应环境信号。STAT5指两种高度相关的蛋白质,即STAT5A和STAT5B,它们具有关键功能:在小鼠中,其完全缺失是致命的;在人类中,仅STAT5B缺失会导致内分泌和免疫问题,而STAT5A缺失尚未见报道。STAT5A和STAT5B的肽序列相似性大于90%,但细微的结构差异表明它们在基因调控中可能具有非冗余作用。然而,这些作用在人类中仍不清楚。我们应用染色质免疫沉淀后进行DNA测序,利用人类CD4(+) T细胞检测由STAT5A和/或STAT5B调控的候选基因,并在STAT5A或STAT5B敲低(KD)的人类CD4(+) T细胞中进行定量PCR以验证结果。我们的数据表明,STAT5A和STAT5B通过与SGK1相互作用在细胞增殖和凋亡中发挥冗余作用。有趣的是,我们发现STAT5A在结合参与神经发育和功能的基因(NDRG1、DNAJC6和SSH2)方面具有一种新的独特作用,而STAT5B似乎通过与DOCK8、SNX9、FOXP3和IL2RA结合在T细胞发育和功能中发挥不同作用。我们的结果还表明,STAT5A和/或STAT5B的一种或多种共激活因子可能在建立不同的结合能力和基因调控行为中发挥重要作用。这些由STAT5A和/或STAT5B调控的基因的新发现对于理解癌症进展、神经疾病和免疫异常的病理生理学具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4598/3907443/cc9ad59160c5/pone.0086790.g001.jpg

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