Cancers (Jun 2024)

Purinergic Ca<sup>2+</sup> Signaling as a Novel Mechanism of Drug Tolerance in BRAF-Mutant Melanoma

  • Philip E. Stauffer,
  • Jordon Brinkley,
  • David A. Jacobson,
  • Vito Quaranta,
  • Darren R. Tyson

DOI
https://doi.org/10.3390/cancers16132426
Journal volume & issue
Vol. 16, no. 13
p. 2426

Abstract

Read online

Drug tolerance is a major cause of relapse after cancer treatment. Despite intensive efforts, its molecular basis remains poorly understood, hampering actionable intervention. We report a previously unrecognized signaling mechanism supporting drug tolerance in BRAF-mutant melanoma treated with BRAF inhibitors that could be of general relevance to other cancers. Its key features are cell-intrinsic intracellular Ca2+ signaling initiated by P2X7 receptors (purinergic ligand-gated cation channels) and an enhanced ability for these Ca2+ signals to reactivate ERK1/2 in the drug-tolerant state. Extracellular ATP, virtually ubiquitous in living systems, is the ligand that can initiate Ca2+ spikes via P2X7 channels. ATP is abundant in the tumor microenvironment and is released by dying cells, ironically implicating treatment-initiated cancer cell death as a source of trophic stimuli that leads to ERK reactivation and drug tolerance. Such a mechanism immediately offers an explanation of the inevitable relapse after BRAFi treatment in BRAF-mutant melanoma and points to actionable strategies to overcome it.

Keywords