Electrical activity between skin cells regulates melanoma initiation

Author:

Tagore MohitaORCID,Hergenreder Emiliano,Suresh Shruthy,Baron Maayan,Perlee Sarah C.,Melendez Stephanie,Hollmann Travis J.,Ideker TreyORCID,Studer Lorenz,White Richard M.

Abstract

SummaryOncogenes can only initiate tumors in certain cellular contexts, which is referred to as oncogenic competence. In melanoma, whether cells in the microenvironment can endow such competence remains unclear. Using a combination of zebrafish transgenesis coupled with human tissues, we demonstrate that GABAergic signaling between keratinocytes and melanocytes promotes melanoma initiation by BRAFV600E. GABA is synthesized in melanoma cells, which then acts on GABA-A receptors on keratinocytes. Electron microscopy demonstrates synapse-like structures between keratinocytes and melanoma cells, and multi-electrode array analysis shows that GABA acts to inhibit electrical activity in melanoma/keratinocyte co-cultures. Genetic and pharmacologic perturbation of GABA synthesis abrogates melanoma initiation in vivo. These data suggest that electrical activity across the skin microenvironment determines the ability of oncogenes to initiate melanoma.

Publisher

Cold Spring Harbor Laboratory

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