Na_v1.5 regulates breast tumor growth and metastatic dissemination in vivo

Michaela Nelson, Ming Yang, Rebecca Millican-Slater and William J. Brackenbury _

Abstract

ABSTRACT

Voltage-gated Na⁺ channels (VGSCs) mediate action potential firing and regulate adhesion and migration in excitable cells. VGSCs are also expressed in cancer cells. In metastatic breast cancer (BCa) cells, the Na_v1.5 α subunit potentiates migration and invasion. In addition, the VGSC-inhibiting antiepileptic drug phenytoin inhibits tumor growth and metastasis. However, the functional activity of Na_v1.5 and its specific contribution to tumor progression in vivo has not been delineated. Here, we found that Na_v1.5 is up-regulated at the protein level in BCa compared with matched normal breast tissue. Na⁺ current, reversibly blocked by tetrodotoxin, was retained in cancer cells in tumor tissue slices, thus directly confirming functional VGSC activity in vivo. Stable down-regulation of Na_v1.5 expression significantly reduced tumor growth, local invasion into surrounding tissue, and metastasis to liver, lungs and spleen in an orthotopic BCa model. Na_v1.5 down-regulation had no effect on cell proliferation or angiogenesis within the in tumors, but increased apoptosis. In vitro, Na_v1.5 down-regulation altered cell morphology and reduced CD44 expression, suggesting that VGSC activity may regulate cellular invasion via the CD44-src-cortactin signaling axis. We conclude that Na_v1.5 is functionally active in cancer cells in breast tumors, enhancing growth and metastatic dissemination. These findings support the notion that compounds targeting Na_v1.5 may be useful for reducing metastasis.

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