Methylated DNA Binding Domain Protein 2 (MBD2) Coordinately Silences Gene Expression through Activation of the MicroRNA hsa-mir-496 Promoter in Breast Cancer Cell Line
Methylated DNA binding protein 2 (MBD2) binds methylated promoters and suppresses transcription in cis through recruitment of a chromatin modification repressor complex. We show here a new mechanism of action for MBD2: suppression of gene expression indirectly through activation of microRNA hsa-mir-496. Overexpression of MBD2 in breast epithelial cell line MCF-10A results in induced expression and demethylation of hsa-mir-496 while depletion of MBD2 in a human breast cancer cell lines MCF-7 and MDA-MB231 results in suppression of hsa-mir-496. Activation of hsa-mir-496 by MBD2 is associated with silencing of several of its target genes while depletion of MBD2 leads to induction of hsa-mir-496 target genes. Depletion of hsa-mir-496 by locked nucleic acid (LNA) antisense oligonucleotide leads to activation of these target genes in MBD2 overexpressing cells supporting that hsa-mir-496 is mediating in part the effects of MBD2 on gene expression. We demonstrate that MBD2 binds the promoter of hsa-mir-496 in MCF-10A, MCF-7 and MDA-MB-231 cells and that it activates an in vitro methylated hsa-mir-496 promoter driving a CG-less luciferase reporter in a transient transfection assay. The activation of hsa-mir-496 is associated with reduced methylation of the promoter. Taken together these results describe a novel cascade for gene regulation by DNA methylation whereby activation of a methylated microRNA by MBD2 that is associated with loss of methylation triggers repression of downstream targets.
机构:
Tokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Aoki, Kazuhisa
;
Sato, Noriko
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Tokyo Med & Dent Univ, Med Res Inst, Dept Mol Epidemiol, Tokyo, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Sato, Noriko
;
Yamaguchi, Atsumi
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Tokyo Metropolitan Inst Publ Hlth, Dept Environm Hlth & Toxicol, Tokyo 1690073, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Yamaguchi, Atsumi
;
Kaminuma, Osamu
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Tokyo Metropolitan Inst Med Sci, Allergy & Immunol Project, Tokyo 1138613, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Kaminuma, Osamu
;
Hosozawa, Takumi
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Tokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Hosozawa, Takumi
;
Miyatake, Shoichiro
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Tokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
机构:
Tokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Aoki, Kazuhisa
;
Sato, Noriko
论文数: 0引用数: 0
h-index: 0
机构:
Tokyo Med & Dent Univ, Med Res Inst, Dept Mol Epidemiol, Tokyo, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Sato, Noriko
;
Yamaguchi, Atsumi
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h-index: 0
机构:
Tokyo Metropolitan Inst Publ Hlth, Dept Environm Hlth & Toxicol, Tokyo 1690073, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Yamaguchi, Atsumi
;
Kaminuma, Osamu
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h-index: 0
机构:
Tokyo Metropolitan Inst Med Sci, Allergy & Immunol Project, Tokyo 1138613, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Kaminuma, Osamu
;
Hosozawa, Takumi
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h-index: 0
机构:
Tokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan
Hosozawa, Takumi
;
Miyatake, Shoichiro
论文数: 0引用数: 0
h-index: 0
机构:
Tokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, JapanTokyo Metropolitan Inst Med Sci, Cytokine Project, Tokyo 1138613, Japan