The Antitumor Effect of Metformin Is Mediated by miR-26a in Breast Cancer

Paula Cabello; Begoña Pineda; Eduardo Tormo; Ana Lluch; Pilar Eroles

doi:10.3390/ijms17081298

The Antitumor Effect of Metformin Is Mediated by miR-26a in Breast Cancer

Int J Mol Sci. 2016 Aug 10;17(8):1298. doi: 10.3390/ijms17081298.

Authors

Paula Cabello¹, Begoña Pineda², Eduardo Tormo³, Ana Lluch^{4

5}, Pilar Eroles⁶

Affiliations

¹ Biomedical Research Institute INCLIVA, 46010 Valencia, Spain. paucanavarro@gmail.com.
² Biomedical Research Institute INCLIVA, 46010 Valencia, Spain. bepime@hotmail.com.
³ Biomedical Research Institute INCLIVA, 46010 Valencia, Spain. eduardo.tormo@uv.es.
⁴ Biomedical Research Institute INCLIVA, 46010 Valencia, Spain. lluch_ana@gva.es.
⁵ Oncology and Hematology Department, Hospital Clinico Universitario, 46010 Valencia, Spain. lluch_ana@gva.es.
⁶ Biomedical Research Institute INCLIVA, 46010 Valencia, Spain. pilar.eroles@uv.es.

Abstract

Metformin, a drug approved for diabetes type II treatment, has been associated with a reduction in the incidence of breast cancer and metastasis and increased survival in diabetic breast cancer patients. High levels of miR-26a expression have been proposed as one of the possible mechanisms for this effect; likewise, this miRNA has also been associated with survival/apoptosis processes in breast cancer. Our aim was to evaluate if miR-26a and some of its targets could mediate the effect of metformin in breast cancer. The viability of MDA-MB-231, MDA-MB-468, and MCF-7 breast cancer cell lines was evaluated with an MTT assay after ectopic overexpression and/or downregulation of miR-26a. Similarly, the expression levels of the miR-26a targets CASP3, CCNE2, ABL2, APAF1, XIAP, BCL-2, PTEN, p53, E2F3, CDC25A, BCL2L1, MCL-1, EZH2, and MTDH were assessed by quantitative polymerase chain reaction (PCR). The effect of metformin treatment on breast cancer cell viability and miR-26a, BCL-2, PTEN, MCL-1, EZH2, and MTDH modulation were evaluated. Wound healing experiments were performed to analyze the effect of miR-26a and metformin treatment on cell migration. MiR-26a overexpression resulted in a reduction in cell viability that was partially recovered by inhibiting it. E2F3, MCL-1, EZH2, MTDH, and PTEN were downregulated by miR-26a and the PTEN (phosphatase and tensin homolog) protein was also reduced after miR-26a overexpression. Metformin treatment reduced breast cancer cell viability, increased miR-26a expression, and led to a reduction in BCL-2, EZH2, and PTEN expression. miR-26a inhibition partly prevents the metformin viability effect and the PTEN and EZH2 expression reduction. Our results indicate that metformin effectively reduces breast cancer cell viability and suggests that the effects of the drug are mediated by an increase in miR-26a expression and a reduction of its targets, PTEN and EHZ2 Thus, the use of metformin in breast cancer treatment constitutes a promising potential breast cancer therapy.

Keywords: breast cancer; metformin; miR-26a.

MeSH terms

Apoptosis / drug effects
Breast Neoplasms / genetics*
Cell Line, Tumor
Cell Survival / drug effects
Cyclins / metabolism
DNA-Binding Proteins / metabolism
Female
Gene Expression Regulation, Neoplastic / drug effects
Humans
Hypoglycemic Agents / pharmacology*
MCF-7 Cells
Metformin / pharmacology*
MicroRNAs / genetics
MicroRNAs / metabolism*
PTEN Phosphohydrolase / metabolism

Substances

CCNE2 protein, human
Cyclins
DNA-Binding Proteins
Hypoglycemic Agents
MIRN26A microRNA, human
MicroRNAs
Metformin
PTEN Phosphohydrolase
PTEN protein, human