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Literature DB >> 27612013

Silencing the epigenetic silencer KDM4A for TRAIL and DR5 simultaneous induction and antitumor therapy.

Junjian Wang¹, Haibin Wang², Ling-Yu Wang¹, Demin Cai¹, Zhijian Duan¹, Yanhong Zhang³, Peng Chen², June X Zou¹, Jianzhen Xu⁴, Xinbin Chen³, Hsing-Jien Kung^1,5, Hong-Wu Chen^1,6.

Abstract

Recombinant TRAIL and agonistic antibodies to death receptors (DRs) have been in clinical trial but displayed limited anti-cancer efficacy. Lack of functional DR expression in tumors is a major limiting factor. We report here that chromatin regulator KDM4A/JMJD2A, not KDM4B, has a pivotal role in silencing tumor cell expression of both TRAIL and its receptor DR5. In TRAIL-sensitive and -resistant cancer cells of lung, breast and prostate, KDM4A small-molecule inhibitor compound-4 (C-4) or gene silencing strongly induces TRAIL and DR5 expression, and causes TRAIL-dependent apoptotic cell death. KDM4A inhibition also strongly sensitizes cells to TRAIL. C-4 alone potently inhibits tumor growth with marked induction of TRAIL and DR5 expression in the treated tumors and effectively sensitizes them to the newly developed TRAIL-inducer ONC201. Mechanistically, C-4 does not appear to act through the Akt-ERK-FOXO3a pathway. Instead, it switches histone modifying enzyme complexes at promoters of TRAIL and DR5 transcriptional activator CHOP gene by dissociating KDM4A and nuclear receptor corepressor (NCoR)-HDAC complex and inducing the recruitment of histone acetylase CBP. Thus, our results reveal KDM4A as a key epigenetic silencer of TRAIL and DR5 in tumors and establish inhibitors of KDM4A as a novel strategy for effectively sensitizing tumors to TRAIL pathway-based therapeutics.

Entities: Disease Gene

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Year: 2016 PMID： 27612013 PMCID： PMC5071577 DOI： 10.1038/cdd.2016.92

Source DB: PubMed Journal: Cell Death Differ ISSN： 1350-9047 Impact factor: 15.828

56 in total

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4. Small-Molecule ONC201/TIC10 Targets Chemotherapy-Resistant Colorectal Cancer Stem-like Cells in an Akt/Foxo3a/TRAIL-Dependent Manner.

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10. ROR-γ drives androgen receptor expression and represents a therapeutic target in castration-resistant prostate cancer.

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Review 3. The Emerging Role of H3K9me3 as a Potential Therapeutic Target in Acute Myeloid Leukemia.

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Review 4. Mechanistic insights into KDM4A driven genomic instability.

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5. Targeting castration-resistant prostate cancer with a novel RORγ antagonist elaiophylin.

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7. KDM4B is a coactivator of c-Jun and involved in gastric carcinogenesis.

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Review 8. Zinc-finger proteins in health and disease.

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Journal: Cell Death Discov Date: 2017-11-13

8 in total