Sam68 Mediates the Activation of Insulin and Leptin Signalling in Breast Cancer Cells.

Antonio Pérez-Pérez,Juan A Virizuela,Teresa Vilariño-García,Luis De La Cruz,Víctor Sánchez-Margalet,Flora Sánchez-Jiménez,Ming Tan

doi:10.1371/journal.pone.0158218

Abstract

Obesity is a well-known risk factor for breast cancer development in postmenopausal women. High insulin and leptin levels seem to have a role modulating the growth of these tumours. Sam68 is an RNA-binding protein with signalling functions that has been found to be overexpressed in breast cancer. Moreover, Sam68 may be recruited to insulin and leptin signalling pathways, mediating its effects on survival, growth and proliferation in different cellular types. We aimed to study the expression of Sam68 and its phosphorylation level upon insulin and leptin stimulation, and the role of Sam68 in the proliferative effect and signalling pathways that are activated by insulin or leptin in human breast adenocarcinoma cells. In the human breast adenocarcinoma cell lines MCF7, MDA-MB-231 and BT-474, Sam68 protein quantity and gene expression were increased upon leptin or insulin stimulation, as it was checked by qPCR and immunoblot. Moreover, both insulin and leptin stimulation promoted an increase in Sam68 tyrosine phosphorylation and negatively regulated its RNA binding capacity. siRNA was used to downregulate Sam68 expression, which resulted in lower proliferative effects of both insulin and leptin, as well as a lower activation of MAPK and PI3K pathways promoted by both hormones. These effects may be partly explained by the decrease in IRS-1 expression by down-regulation of Sam68. These results suggest the participation of Sam68 in both leptin and insulin receptor signaling in human breast cancer cells, mediating the trophic effects of these hormones in proliferation and cellular growth.

Highlights

Sam68, known as KHDRBS1 (KH domain-containing, RNA-binding, signal-transductionassociated 1) is a member of the signal transduction activator of RNA (STAR) family of RNAbinding proteins (RBPs)
According to the previously described participation of Sam68 in insulin and leptin signalling [8], we aim to study the role of this protein in the signal transduction pathways that are activated by leptin and insulin to mediate their proliferative effect in breast cancer cells
In order to check the effect of leptin and insulin on Sam68 expression in the three adenocarcinoma cell lines, they were independently incubated in the absence of serum with and without leptin or insulin (1 nM) for 24 h

Summary

Introduction

Known as KHDRBS1 (KH domain-containing, RNA-binding, signal-transductionassociated 1) is a member of the signal transduction activator of RNA (STAR) family of RNAbinding proteins (RBPs). According to the role of Sam as an RNA binding protein, it has been described that this protein modulates several steps of RNA metabolism [3], such as nuclear export and cytoplasmic utilization or translation of viral and cellular mRNAs [4,5] and regulation of alternative splicing, where Sam plays a key role [6]. This protein has been described as a scaffold protein recruited in various signal transduction pathways [7,8] linking signalling pathways and RNA metabolism regulation. RNA binding ability and localization are regulated by phosphorylation and other posttranslational modifications [11,12,13,14,15]

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