Downregulation of the tumor-suppressor miR-16 via progestin-mediated oncogenic signaling contributes to breast cancer development

Downregulation of the tumor-suppressor miR-16 via progestin-mediated oncogenic signaling contributes to breast cancer development

Experimental and clinical evidence points to a critical role of progesterone and the nuclear progesterone receptor (PR) in controlling mammary gland tumorigenesis. However, the molecular mechanisms of progesterone action in breast cancer still remain elusive. On the other hand, micro RNAs (miRNAs) a...

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Bibliographic Details
Published in:Breast cancer research : BCR Vol. 14; no. 3; p. R77
Main Authors: Rivas, Martin A, Venturutti, Leandro, Huang, Yi-Wen, Schillaci, Roxana, Huang, Tim Hui-Ming, Elizalde, Patricia V
Format: Journal Article
Language:English
Published: England BioMed Central Ltd 14-05-2012
BioMed Central
Subjects:
3' Untranslated regions
3' Untranslated Regions - genetics
Acids
Analysis
Animals
Breast cancer
Breast Neoplasms - genetics
Breast Neoplasms - metabolism
c-Myc protein
Cell cycle
Cell Line, Tumor
Cell Proliferation
Cyclin E
Cyclin E - genetics
Cyclin E - metabolism
Development and progression
Down-Regulation
ErbB protein
Female
Gene Expression Regulation, Neoplastic
Genes, Tumor Suppressor
Genome-Wide Association Study
Genomics
heregulin
Humans
Leukemia
Mammary gland
Mice
Mice, Inbred BALB C
MicroRNA
MicroRNAs - metabolism
miRNA
Molecular modelling
Oncogene Proteins - genetics
Oncogene Proteins - metabolism
Physiological aspects
Progestational hormones
Progesterone
Progesterone receptors
progestin
Progestins - metabolism
Proteins - metabolism
Proto-Oncogene Proteins c-myc - genetics
Proto-Oncogene Proteins c-myc - metabolism
Receptors, Progesterone - genetics
Receptors, Progesterone - metabolism
Reporter gene
RNA Interference
RNA, Small Interfering
Signal Transduction
Stat3 protein
STAT3 Transcription Factor - genetics
STAT3 Transcription Factor - metabolism
Transcription factors
Tumor cell lines
Tumor cells
Tumor suppressor genes
Tumorigenesis
Up-Regulation
Western blotting
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Summary:Experimental and clinical evidence points to a critical role of progesterone and the nuclear progesterone receptor (PR) in controlling mammary gland tumorigenesis. However, the molecular mechanisms of progesterone action in breast cancer still remain elusive. On the other hand, micro RNAs (miRNAs) are short ribonucleic acids which have also been found to play a pivotal role in cancer pathogenesis. The role of miRNA in progestin-induced breast cancer is poorly explored. In this study we explored progestin modulation of miRNA expression in mammary tumorigenesis. We performed a genome-wide study to explore progestin-mediated regulation of miRNA expression in breast cancer. miR-16 expression was studied by RT-qPCR in cancer cell lines with silenced PR, signal transducer and activator of transcription 3 (Stat3) or c-Myc, treated or not with progestins. Breast cancer cells were transfected with the precursor of miR-16 and proliferation assays, Western blots or in vivo experiments were performed. Target genes of miR-16 were searched through a bioinformatical approach, and the study was focused on cyclin E. Reporter gene assays were performed to confirm that cyclin E 3'UTR is a direct target of miR-16. We found that nine miRNAs were upregulated and seven were downregulated by progestin in mammary tumor cells. miR-16, whose function as a tumor suppressor in leukemia has already been shown, was identified as one of the downregulated miRNAs in murine and human breast cancer cells. Progestin induced a decrease in miR-16 levels via the classical PR and through a hierarchical interplay between Stat3 and the oncogenic transcription factor c-Myc. A search for miR-16 targets showed that the CCNE1 gene, encoding the cell cycle regulator cyclin E, contains conserved putative miR-16 target sites in its mRNA 3' UTR region. We found that, similar to the molecular mechanism underlying progestin-modulated miR-16 expression, Stat3 and c-Myc participated in the induction of cyclin E expression by progestin. Moreover, overexpression of miR-16 abrogated the ability of progestin to induce cyclin E upregulation, revealing that cyclin E is a novel target of miR-16 in breast cancer. Overexpression of miR-16 also inhibited progestin-induced breast tumor growth in vitro and in vivo, demonstrating for the first time, a role for miR-16 as a tumor suppressor in mammary tumorigenesis. We also found that the ErbB ligand heregulin (HRG) downregulated the expression of miR-16, which then participates in the proliferative activity of HRG in breast tumor cells. In this study, we reveal the first progestin-regulated miRNA expression profile and identify a novel role for miR-16 as a tumor suppressor in progestin- and growth factor-induced growth in breast cancer.
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content type line 23
ISSN:1465-542X
1465-5411
1465-542X
DOI:10.1186/bcr3187