Abstract
BackgroundMetformin, an FDA-approved drug for the treatment of Type II diabetes, has emerged as a promising anti-cancer agent. Other biguanide analogs, including buformin and phenformin, are suggested to have similar properties. Although buformin was shown to reduce mammary tumor burden in carcinogen models, the anti-cancer effects of buformin on different breast cancer subtypes and the underlying mechanisms remain unclear. Therefore, we aimed to investigate the effects of buformin on erbB-2-overexpressing breast cancer with in vitro and in vivo models.MethodsMTT, cell cycle, clonogenic/CFC, ALDEFLUOR, tumorsphere, and Western blot analyses were used to determine the effects of buformin on cell growth, stem cell populations, stem cell-like properties, and signaling pathways in SKBR3 and BT474 erbB-2-overexpressing breast cancer cell lines. A syngeneic tumor cell transplantation model inoculating MMTV-erbB-2 mice with 78617 mouse mammary tumor cells was used to study the effects of buformin (1.2 g buformin/kg chow) on tumor growth in vivo. MMTV-erbB-2 mice were also fed buformin for 10 weeks, followed by analysis of premalignant mammary tissues for changes in morphological development, mammary epithelial cell (MEC) populations, and signaling pathways.ResultsBuformin significantly inhibited SKBR3 and BT474 cell growth, and in vivo activity was demonstrated by considerable growth inhibition of syngeneic tumors derived from MMTV-erbB-2 mice. In particular, buformin suppressed stem cell populations and self-renewal in vitro, which was associated with inhibited receptor tyrosine kinase (RTK) and mTOR signaling. Consistent with in vitro data, buformin suppressed mammary morphogenesis and reduced cell proliferation in MMTV-erbB-2 mice. Importantly, buformin decreased MEC populations enriched with mammary reconstitution units (MRUs) and tumor-initiating cells (TICs) from MMTV-erbB-2 mice, as supported by impaired clonogenic and mammosphere formation in primary MECs. We further demonstrated that buformin-mediated in vivo inhibition of MEC stemness is associated with suppressed activation of mTOR, RTK, ER, and β-catenin signaling pathways.ConclusionsOverall, our results provide evidence for buformin as an effective anti-cancer drug that selectively targets TICs, and present a novel prevention and/or treatment strategy for patients who are genetically predisposed to erbB-2-overexpressing breast cancer.
Highlights
Metformin, an FDA-approved drug for the treatment of Type II diabetes, has emerged as a promising anti-cancer agent
Buformin inhibits cell proliferation and induces cell cycle arrest in erbB-2-overexpressing breast cancer cells in vitro Metformin has demonstrated the capability to inhibit cell proliferation in various cancer cells, yet previous reports have shown that phenformin and buformin have increased biological activity than metformin [31]
We found that buformin reduced cell viability in erbB-2-overexpressing SKBR3 (IC50 = 246.7 μM) and BT474 (IC50 = 98.6 μM) breast cancer cell lines (Fig. 1a)
Summary
An FDA-approved drug for the treatment of Type II diabetes, has emerged as a promising anti-cancer agent. Buformin was shown to reduce mammary tumor burden in carcinogen models, the anti-cancer effects of buformin on different breast cancer subtypes and the underlying mechanisms remain unclear. Metformin, a biguanide drug commonly prescribed to treat Type II diabetes in humans, has demonstrated anti-cancer effects, which was published in an earlier milestone report by Evans et al (2005) showing that metformin significantly reduced the risk of developing multiple types of cancer in patients with diabetes [3]. Breast cancers, including the erbB-2-overexpressing subtype, are often associated with morbidity and poor clinical outcomes; the identification and development of effective erbB-2overexpressing breast cancer prevention and treatment options are crucial [5,6,7]
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