4.5 Article

Chromatin reader ZMYND8 is a key target of all trans retinoic acid-mediated inhibition of cancer cell proliferation

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ELSEVIER
DOI: 10.1016/j.bbagrm.2017.02.004

关键词

ZMYND8; Chromatin reader; Histone modifications; Retinoic acid; Gene regulation; Cell proliferation

资金

  1. Department of Atomic Energy (DAE), Govt. of India [12-RD-SIN-5.04-0103]
  2. Science & Engineering Research Board (SERB) by Department of Science and Technology (DST), Govt. of India [EMR/2014/000335]
  3. Department of Biotechnology (DBT)
  4. INSPIRE-faculty scheme of Department of Science and Technology (DST), Govt. of India

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All trans retinoic acid (ATRA), an active vitamin-A derivative, has been shown to regulate gene expression program and thus imparts anti-proliferative activity to cancer cells. Previously, we identified a dual histone reader ZMYND8 (zinc finger MYND (Myeloid, Nervy and DEAF-1)-type containing 8), to be a novel target of ATRA. In the present study, we attempted to decipher the detail mechanism of its transcription regulation. ATRA can reprogram the epigenetic landscape in the upstream regulatory region of ZMYND8 thereby promoting its expression. Interestingly, there is a unique H31<27Me3 to H3K27Ac switch upon ATRA-treatment. We show here that ATRA causes dynamic changes in recruitment of transcription factor YY1 in concert with HDAC1 at ZMYND8 promoter. Further, we show that ATRA treatment triggers an anti-proliferative activity in cancer cells through regulation of ZMYND8 expression. Subsequently, in 4T1-induced syngenic tumor mouse model, ATRA injection caused significant upregulation of ZMYND8. Overall our findings highlight a novel mechanism underlying ATRA-mediated changes in ZMYND8 expression which, in turn, activates the anti-proliferative program in a cancer cell. Thus, histone reader mediated modulation of epigenetic language could play a significant role in retinoid based therapeutic strategy which is well exploited to combat tumor growth. (C) 2017 Elsevier B.V. All rights reserved.

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