The Endogenous Retrovirus-derived Long Noncoding RNA TROJAN Promotes Triple-negative Breast Cancer Progression Via ZMYND8 Degradation

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2019 Mar 12

PMID 30854423

Citations 63

Authors

Xi Jin

Xiao-En Xu

Yi-Zhou Jiang

Yi-Rong Liu

Wei Sun

Ya-Jie Guo

Yi-Xing Ren

Wen-Jia Zuo

Xin Hu

Sheng-Lin Huang

Hong-Jie Shen

Fei Lan

Yun-Fei He

Guo-Hong Hu

Gen-Hong Di

Xiang-Huo He

Da-Qiang Li

Suling Liu

Ke-Da Yu

Zhi-Ming Shao

Affiliations

Soon will be listed here.

Abstract

Human endogenous retroviruses (HERVs) play pivotal roles in the development of breast cancer. However, the detailed mechanisms of noncoding HERVs remain elusive. Here, our genome-wide transcriptome analysis of HERVs revealed that a primate long noncoding RNA, which we dubbed TROJAN, was highly expressed in human triple-negative breast cancer (TNBC). TROJAN promoted TNBC proliferation and invasion and indicated poor patient outcomes. We further confirmed that TROJAN could bind to ZMYND8, a metastasis-repressing factor, and increase its degradation through the ubiquitin-proteasome pathway by repelling ZNF592. TROJAN also epigenetically up-regulated metastasis-related genes in multiple cell lines. Correlations between TROJAN and ZMYND8 were subsequently confirmed in clinical samples. Furthermore, our study verified that antisense oligonucleotide therapy targeting TROJAN substantially suppressed TNBC progression in vivo. In conclusion, the long noncoding RNA TROJAN promotes TNBC progression and serves as a potential therapeutic target.

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