Crif1是信号转导及转录激活因子3（STAT3）的一种新型转录共激活因子。

Crif1 is a novel transcriptional coactivator of STAT3.

作者信息

Kwon Min-chul, Koo Bon-Kyoung, Moon Jin-Sook, Kim Yoon-Young, Park Ki Cheol, Kim Nam-Shik, Kwon Mi Yi, Kong Myung-Phil, Yoon Ki-Jun, Im Sun-Kyoung, Ghim Jaewang, Han Yong-Mahn, Jang Sung Key, Shong Minho, Kong Young-Yun

机构信息

Department of Life Science, Division of Molecular and Life Sciences, Pohang University of Science and Technology, Pohang, South Korea.

出版信息

EMBO J. 2008 Feb 20;27(4):642-53. doi: 10.1038/sj.emboj.7601986. Epub 2008 Jan 17.

DOI:10.1038/sj.emboj.7601986

PMID:18200042

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2262042/

Abstract

Signal transducer and activator of transcription 3 (STAT3) is a transcriptional factor that performs a broad spectrum of biological functions in response to various stimuli. However, no specific coactivator that regulates the transcriptional activity of STAT3 has been identified. Here we report that CR6-interacting factor 1 (Crif1) is a specific transcriptional coactivator of STAT3, but not of STAT1 or STAT5a. Crif1 interacts with STAT3 and positively regulates its transcriptional activity. Crif1-/- embryos were lethal around embryonic day 6.5, and manifested developmental arrest accompanied with defective proliferation and massive apoptosis. The expression of STAT3 target genes was markedly reduced in a Crif1-/- blastocyst culture and in Oncostatin M-stimulated Crif1-deficient MEFs. Importantly, the key activities of constitutively active STAT3-C, such as transcription, DNA binding, and cellular transformation, were abolished in the Crif1-null MEFs, suggesting the essential role of Crif1 in the transcriptional activity of STAT3. Our results reveal that Crif1 is a novel and essential transcriptional coactivator of STAT3 that modulates its DNA binding ability, and shed light on the regulation of oncogenic STAT3.

摘要

信号转导与转录激活因子3（STAT3）是一种转录因子，可响应各种刺激发挥广泛的生物学功能。然而，尚未鉴定出调节STAT3转录活性的特异性共激活因子。在此我们报告，CR6相互作用因子1（Crif1）是STAT3的特异性转录共激活因子，而非STAT1或STAT5a的转录共激活因子。Crif1与STAT3相互作用并正向调节其转录活性。Crif1基因敲除胚胎在胚胎第6.5天左右致死，并表现出发育停滞，伴有增殖缺陷和大量细胞凋亡。在Crif1基因敲除囊胚培养物和抑瘤素M刺激的Crif1缺陷型小鼠胚胎成纤维细胞（MEF）中，STAT3靶基因的表达明显降低。重要的是，组成型激活的STAT3-C的关键活性，如转录、DNA结合和细胞转化，在Crif1基因敲除的MEF中被消除，这表明Crif1在STAT3转录活性中起重要作用。我们的结果表明，Crif1是一种新型且必需的STAT3转录共激活因子，可调节其DNA结合能力，并为致癌性STAT3的调控提供了线索。

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