Cooperation of ATF4 and CTCF promotes adipogenesis through transcriptional regulation

CTCF公司 脂肪生成 转录因子 细胞生物学 脂肪组织 生物 增强子 ATF4 癌症研究 基因 遗传学 内分泌学 间充质干细胞
作者
Ying‐Chun Chen,Rong‐Quan He,Zhiqiang Han,Yanyan Wu,Qiuyan Wang,Xiujuan Zhu,Zhi‐Guang Huang,Juan Ye,Yao Tang,Hongbin Huang,Jianxu Chen,Hong Shan,Fei Xiao
出处
期刊:Cell Biology and Toxicology [Springer Science+Business Media]
卷期号:38 (5): 741-763 被引量:22
标识
DOI:10.1007/s10565-021-09608-x
摘要

Adipogenesis is a multi-step process orchestrated by activation of numerous TFs, whose cooperation and regulatory network remain elusive. Activating transcription factor 4 (ATF4) is critical for adipogenesis, yet its regulatory network is unclarified. Here, we mapped genome-wide ATF4 binding landscape and its regulatory network by Chip-seq and RNA-seq and found ATF4 directly modulated transcription of genes enriching in fat cell differentiation. Motifs of TFs especially CTCF were found from ATF4 binding sites, suggesting a direct role of ATF4 in regulating adipogenesis associated with CTCF and other TFs. Deletion of CTCF attenuated adipogenesis while overexpression enhanced adipocyte differentiation, indicating CTCF is indispensable for adipogenesis. Intriguingly, combined analysis of Chip-seq data of these two TFs showed that ATF4 co-localized with CTCF in the promoters of key adipogenic genes including Cebpd and PPARg and co-regulated their transactivation. Moreover, ATF4 directly regulated CTCF expression and interacted with CTCF in differentiated 3T3-L1 cells. In vivo, downregulation of ATF4 suppressed the expression of CTCF, Cebpd, and PPARg, leading to reduced adipose tissue expansion in refeeding mice. Consistently, mRNA expression of ATF4 and CTCF was positively correlated with each other in human subcutaneous adipose tissue and inversely associated with BMI, indicating a possible involvement of these two TFs in adipose development. Taken together, our data propose for the first time that ATF4 and CTCF work cooperatively to control adipogenesis and adipose development via orchestrating transcription of adipogenic genes. Our findings reveal novel therapeutic targets in obesity treatment.
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