Amplification of a Calcium Channel Subunit CACNG4 Increases Breast Cancer Metastasis

Overview

Journal EBioMedicine

Specialty Biomedical Engineering

Date 2020 Feb 17

PMID 32062352

Citations 27

Authors

Nisha Kanwar

Katia Carmine-Simmen

Ranju Nair

Chunjie Wang

Soode Moghadas-Jafari

Heiko Blaser

Danh Tran-Thanh

Dongyu Wang

Peiqi Wang

Jenny Wang

Adrian Pasculescu

Alessandro Datti

Tak Mak

John D Lewis

Susan J Done

Affiliations

Soon will be listed here.

Abstract

Background: Previously, we found that amplification of chromosome 17q24.1-24.2 is associated with lymph node metastasis, tumour size, and lymphovascular invasion in invasive ductal carcinoma. A gene within this amplicon, CACNG4, an L-type voltage-gated calcium channel gamma subunit, is elevated in breast cancers with poor prognosis. Calcium homeostasis is achieved by maintaining low intracellular calcium levels. Altering calcium influx/efflux mechanisms allows tumour cells to maintain homeostasis despite high serum calcium levels often associated with advanced cancer (hypercalcemia) and aberrant calcium signaling.

Methods: In vitro 2-D and 3-D assays, and intracellular calcium influx assays were utilized to measure tumourigenic activity in response to altered CANCG4 levels and calcium channel blockers. A chick-CAM model and mouse model for metastasis confirmed these results in vivo.

Findings: CACNG4 alters cell motility in vitro, induces malignant transformation in 3-dimensional culture, and increases lung-specific metastasis in vivo. CACNG4 functions by closing the channel pore, inhibiting calcium influx, and altering calcium signaling events involving key survival and metastatic pathway genes (AKT2, HDAC3, RASA1 and PKCζ).

Interpretation: CACNG4 may promote homeostasis, thus increasing the survival and metastatic ability of tumour cells in breast cancer. Our findings suggest an underlying pathway for tumour growth and dissemination regulated by CACNG4 that is significant with respect to developing treatments that target these channels in tumours with aberrant calcium signaling.

Funding: Canadian Breast Cancer Foundation, Ontario; Canadian Institutes of Health Research.

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