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CREPT/RPRD1B 通过依赖于 p300 的 STAT3 驱动的基因转录促进肿瘤发生。

CREPT/RPRD1B promotes tumorigenesis through STAT3-driven gene transcription in a p300-dependent manner.

机构信息

State Key Laboratory of Membrane Biology, School of Medicine, Tsinghua University, Beijing, China.

Tsinghua-Peking Joint Center for Life Sciences, School of Life Science, Tsinghua University, Beijing, China.

出版信息

Br J Cancer. 2021 Apr;124(8):1437-1448. doi: 10.1038/s41416-021-01269-1. Epub 2021 Feb 3.

DOI:10.1038/s41416-021-01269-1
PMID:33531691
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8039031/
Abstract

BACKGROUND

Signal transducer and activator of transcription 3 (STAT3) has been shown to upregulate gene transcription during tumorigenesis. However, how STAT3 initiates transcription remains to be exploited. This study is to reveal the role of CREPT (cell cycle-related and elevated-expression protein in tumours, or RPRD1B) in promoting STAT3 transcriptional activity.

METHODS

BALB/c nude mice, CREPT overexpression or deletion cells were employed for the assay of tumour formation, chromatin immunoprecipitation, assay for transposase-accessible chromatin using sequencing.

RESULTS

We demonstrate that CREPT, a recently identified oncoprotein, enhances STAT3 transcriptional activity to promote tumorigenesis. CREPT expression is positively correlated with activation of STAT3 signalling in tumours. Deletion of CREPT led to a decrease, but overexpression of CREPT resulted in an increase, in STAT3-initiated tumour cell proliferation, colony formation and tumour growth. Mechanistically, CREPT interacts with phosphorylated STAT3 (p-STAT3) and facilitates p-STAT3 to recruit p300 to occupy at the promoters of STAT3-targeted genes. Therefore, CREPT and STAT3 coordinately facilitate p300-mediated acetylation of histone 3 (H3K18ac and H3K27ac), further augmenting RNA polymerase II recruitment. Accordingly, depletion of p300 abolished CREPT-enhanced STAT3 transcriptional activity.

CONCLUSIONS

We propose that CREPT is a co-activator of STAT3 for recruiting p300. Our study provides an alternative strategy for the therapy of cancers related to STAT3.

摘要

背景

信号转导子和转录激活子 3(STAT3)已被证明在肿瘤发生过程中上调基因转录。然而,STAT3 如何启动转录仍有待探索。本研究旨在揭示细胞周期相关和肿瘤高表达蛋白(或 RPRD1B)CREPT 在促进 STAT3 转录活性中的作用。

方法

采用 BALB/c 裸鼠、CREPT 过表达或缺失细胞进行肿瘤形成检测、染色质免疫沉淀、测序分析转座酶可及染色质检测。

结果

我们证明了最近被鉴定为癌蛋白的 CREPT 增强 STAT3 转录活性以促进肿瘤发生。CREPT 的表达与肿瘤中 STAT3 信号的激活呈正相关。删除 CREPT 会导致 STAT3 起始的肿瘤细胞增殖、集落形成和肿瘤生长减少,但过表达 CREPT 会导致其增加。从机制上讲,CREPT 与磷酸化 STAT3(p-STAT3)相互作用,并促进 p-STAT3 将 p300 募集到 STAT3 靶向基因的启动子上。因此,CREPT 和 STAT3 协同促进 p300 介导的组蛋白 3(H3K18ac 和 H3K27ac)乙酰化,进一步增加 RNA 聚合酶 II 的募集。因此,p300 的耗竭消除了 CREPT 增强的 STAT3 转录活性。

结论

我们提出 CREPT 是 STAT3 的共激活因子,用于募集 p300。我们的研究为与 STAT3 相关的癌症治疗提供了一种替代策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e065/8039031/eabefed83ea5/41416_2021_1269_Fig1_HTML.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e065/8039031/eabefed83ea5/41416_2021_1269_Fig1_HTML.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e065/8039031/eabefed83ea5/41416_2021_1269_Fig1_HTML.jpg

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