Literature DB >> 26187004

Human DMTF1β antagonizes DMTF1α regulation of the p14(ARF) tumor suppressor and promotes cellular proliferation.

Mario P Tschan1, Elena A Federzoni2, Aladin Haimovici3, Christian Britschgi2, Bettina A Moser4, Jing Jin3, Venkateshwar A Reddy2, Dennis A Sheeter2, Kimberlee M Fischer2, Peiqing Sun5, Bruce E Torbett6.   

Abstract

The human DMTF1 (DMP1) transcription factor, a DNA binding protein that interacts with cyclin D, is a positive regulator of the p14ARF (ARF) tumor suppressor. Our earlier studies have shown that three differentially spliced human DMP1 mRNAs, α, β and γ, arise from the human gene. We now show that DMP1α, β and γ isoforms differentially regulate ARF expression and promote distinct cellular functions. In contrast to DMP1α, DMP1β and γ did not activate the ARF promoter, whereas only β resulted in a dose-dependent inhibition of DMP1α-induced transactivation of the ARF promoter. Ectopic expression of DMP1β reduced endogenous ARF mRNA levels in human fibroblasts. The DMP1β- and γ-isoforms share domains necessary for the inhibitory function of the β-isoform. That DMP1β may interact with DMP1α to antagonize its function was shown in DNA binding assays and in cells by the close proximity of DMP1α/β in the nucleus. Cells stably expressing DMP1β, as well as shRNA targeting all DMP1 isoforms, disrupted cellular growth arrest induced by serum deprivation or in PMA-derived macrophages in the presence or absence of cellular p53. DMP1 mRNA levels in acute myeloid leukemia samples, as compared to granulocytes, were reduced. Treatment of acute promyelocytic leukemia patient samples with all-trans retinoic acid promoted differentiation to granulocytes and restored DMP1 transcripts to normal granulocyte levels. Our findings imply that DMP1α- and β-ratios are tightly regulated in hematopoietic cells and DMP1β antagonizes DMP1α transcriptional regulation of ARF resulting in the alteration of cellular control with a gain in proliferation.
Copyright © 2015 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  ARF; Human DMP1; Human DMTF1; Leukemia; p14(ARF); p53

Mesh:

Substances:

Year:  2015        PMID: 26187004      PMCID: PMC4687731          DOI: 10.1016/j.bbagrm.2015.07.009

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


  52 in total

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3.  Identification of the p53 family-responsive element in the promoter region of the tumor suppressor gene hypermethylated in cancer 1.

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Journal:  Oncogene       Date:  2006-03-30       Impact factor: 9.867

4.  Dmp1 is haplo-insufficient for tumor suppression and modifies the frequencies of Arf and p53 mutations in Myc-induced lymphomas.

Authors:  K Inoue; F Zindy; D H Randle; J E Rehg; C J Sherr
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Authors:  Merel E Lingbeek; Jacqueline J L Jacobs; Maarten van Lohuizen
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Review 6.  p53 and ARF: unexpected players in autophagy.

Authors:  Gregor M Balaburski; Robert D Hontz; Maureen E Murphy
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Authors:  Robert D Kendig; Fumitake Kai; Elizabeth A Fry; Kazushi Inoue
Journal:  Cancer Invest       Date:  2017-04-13       Impact factor: 2.176

3.  Aberrant Expression of p14ARF in Human Cancers: A New Biomarker?

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Journal:  Tumor Microenviron       Date:  2019-02-04

Review 4.  Oncogenic and tumor-suppressive mouse models for breast cancer engaging HER2/neu.

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5.  Clinical applications of mouse models for breast cancer engaging HER2/neu.

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6.  Haploinsufficient tumor suppressor genes.

Authors:  Kazushi Inoue; Elizabeth A Fry
Journal:  Adv Med Biol       Date:  2017 1st Quarter

Review 7.  Aberrant splicing of the DMP1-ARF-MDM2-p53 pathway in cancer.

Authors:  Kazushi Inoue; Elizabeth A Fry
Journal:  Int J Cancer       Date:  2016-02-08       Impact factor: 7.396

8.  MiR-6838-5p facilitates the proliferation and invasion of renal cell carcinoma cells through inhibiting the DMTF1/ARF-p53 axis.

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9.  SRSF5 regulates alternative splicing of DMTF1 pre-mRNA through modulating SF1 binding.

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Review 10.  Novel Molecular Markers for Breast Cancer.

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