PLoS ONE (Jan 2018)

ER-positive breast cancer cells are poised for RET-mediated endocrine resistance.

  • Sachi Horibata,
  • Edward J Rice,
  • Chinatsu Mukai,
  • Brooke A Marks,
  • Kelly Sams,
  • Hui Zheng,
  • Lynne J Anguish,
  • Scott A Coonrod,
  • Charles G Danko

DOI
https://doi.org/10.1371/journal.pone.0194023
Journal volume & issue
Vol. 13, no. 4
p. e0194023

Abstract

Read online

The RET tyrosine kinase signaling pathway is involved in the development of endocrine resistant ER+ breast cancer. However, we know little about how ER+ cells activate RET signaling and initiate an endocrine resistant phenotype. Here we show that both ER+ endocrine resistant and sensitive breast cancers have a functional RET tyrosine kinase signaling pathway, but that endocrine sensitive breast cancer cells lack RET ligands that are necessary to drive endocrine resistance. Transcription of one RET ligand, GDNF, is necessary and sufficient to confer resistance in the ER+ MCF-7 cell line. Endogenous GDNF produced by endocrine resistant cells is translated, secreted into the media, and activates RET signaling in nearby cells. In patients, RET ligand expression predicts responsiveness to endocrine therapies and correlates with survival. Collectively, our findings show that ER+ tumor cells are "poised" for RET mediated endocrine resistance, expressing all components of the RET signaling pathway, but endocrine sensitive cells lack high expression of RET ligands that are necessary to initiate the resistance phenotype.