Literature DB >> 24991827

YY1-MIR372-SQSTM1 regulatory axis in autophagy.

Lifeng Feng1, Yanning Ma1, Jie Sun1, Qi Shen2, Leiming Liu1, Haiqi Lu1, Faliang Wang1, Yongfang Yue1, Jiaqiu Li2, Shenjie Zhang1, Xiaoying Lin1, Jue Chu1, Weidong Han2, Xian Wang2, Hongchuan Jin1.   

Abstract

Autophagy is a self-proteolytic process that degrades intracellular material to enable cellular survival under unfavorable conditions. However, how autophagy is activated in human carcinogenesis remains largely unknown. Herein we report an epigenetic regulation of autophagy in human cancer cells. YY1 (YY1 transcription factor) is a well-known epigenetic regulator and is upregulated in many cancers. We found that YY1 knockdown inhibited cell viability and autophagy flux through downregulating SQSTM1 (sequestosome 1). YY1 regulated SQSTM1 expression through the epigenetic modulation of the transcription of MIR372 (microRNA 372) which was found to target SQSTM1 directly. During nutrient starvation, YY1 was stimulated to promote SQSTM1 expression and subsequent autophagy activation by suppressing MIR372 expression. Similar to YY1 depletion, MIR372 overexpression blocked autophagy activation and inhibited in vivo tumor growth. SQSTM1 upregulation and competent autophagy flux thus contributed to the oncogenic function of YY1. YY1-promoted SQSTM1 upregulation might be a useful histological marker for cancer detection and a potential target for drug development.

Entities:  

Keywords:  MIR372; SQSTM1; YY1; autophagy; epigenetics

Mesh:

Substances:

Year:  2014        PMID: 24991827      PMCID: PMC4203520          DOI: 10.4161/auto.29486

Source DB:  PubMed          Journal:  Autophagy        ISSN: 1554-8627            Impact factor:   16.016


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