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» Articles » PMID: 25219498

Modification of ASC1 by UFM1 is Crucial for ERα Transactivation and Breast Cancer Development

Overview
Journal Mol Cell
Publisher Cell Press
Specialty Cell Biology
Date 2014 Sep 16
PMID 25219498
Citations 100
Authors
Hee Min Yoo
Sung Hwan Kang
Jae Yeon Kim
Joo Eun Lee
Min Woo Seong
Seong Won Lee
Seung Hyeun Ka
Yu-Shin Sou
Masaaki Komatsu
Keiji Tanaka
Soon Tae Lee
Dong Young Noh
Sung Hee Baek
Young Joo Jeon
Chin Ha Chung
Affiliations
Soon will be listed here.
Abstract

Biological roles for UFM1, a ubiquitin-like protein, are largely unknown, and therefore we screened for targets of ufmylation. Here we show that ufmylation of the nuclear receptor coactivator ASC1 is a key step for ERα transactivation in response to 17β-estradiol (E2). In the absence of E2, the UFM1-specific protease UfSP2 was bound to ASC1, which maintains ASC1 in a nonufmylated state. In the presence of E2, ERα bound ASC1 and displaced UfSP2, leading to ASC1 ufmylation. Polyufmylation of ASC1 enhanced association of p300, SRC1, and ASC1 at promoters of ERα target genes. ASC1 overexpression or UfSP2 knockdown promoted ERα-mediated tumor formation in vivo, which could be abrogated by treatment with the anti-breast cancer drug tamoxifen. In contrast, expression of ufmylation-deficient ASC1 mutant or knockdown of the UFM1-activating E1 enzyme UBA5 prevented tumor growth. These findings establish a role for ASC1 ufmylation in breast cancer development by promoting ERα transactivation.

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