Repression of Endometrial Tumor Growth by Targeting SREBP1 and Lipogenesis

Overview

Journal Cell Cycle

Specialty Cell Biology

Date 2012 Jun 8

PMID 22672904

Citations 43

Authors

Weihua Li

YanHong Tai

Jie Zhou

Weiting Gu

Zhaofang Bai

Tao Zhou

Zhijiu Zhong

Peter A McCue

Nianli Sang

Jun-Yuan Ji

Beihua Kong

Jie Jiang

Chenguang Wang

Affiliations

Soon will be listed here.

Abstract

The aberrantly increased lipogenesis is a universal metabolic feature of proliferating tumor cells. Although most normal cells acquire the bulk of their fatty acids from circulation, tumor cells synthesize more than 90% of required lipids de novo. The sterol regulatory element-binding protein 1 (SREBP1), encoded by SREBF1 gene, is a master regulator of lipogenic gene expression. SREBP1 and its target genes are overexpressed in a variety of cancers; however, the role of SREBP1 in endometrial cancer is largely unknown. We have screened a cohort of endometrial cancer (EC) specimen for their lipogenic gene expression and observed a significant increase of SREBP1 target gene expression in cancer cells compared with normal endometrium. By using immunohistochemical staining, we confirmed SREBP1 protein overexpression and demonstrated increased nuclear distribution of SREBP1 in EC. In addition, we found that knockdown of SREBP1 expression in EC cells suppressed cell growth, reduced colonigenic capacity and slowed tumor growth in vivo. Furthermore, we observed that knockdown of SREBP1 induced significant cell death in cultured EC cells. Taken together, our results show that SREBP1 is essential for EC cell growth both in vitro and in vivo, suggesting that SREBP1 activity may be a novel therapeutic target for endometrial cancers.

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