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The heterogeneity of prostate cancers lacking AR activity will require diverse treatment approaches.

Authors :
Labrecque, Mark P.
Alumkal, Joshi J.
Coleman, Ilsa M.
Nelson, Peter S.
Morrissey, Colm
Source :
Endocrine-Related Cancer; Aug2021, Vol. 28 Issue 8, pT51-T66, 16p
Publication Year :
2021

Abstract

The use of androgen deprivation therapy and second-line anti-androgens in prostate cancer has led to the emergence of tumors employing multiple an drogen receptor (AR)-dependent and AR-independent mechanisms to resist AR-targeted therapies in castrationresistant prostate cancer (CRPC). While the AR signaling axis remains the cornerstone for therapeutic development in CRPC, a clearer understanding of the heterogeneous biology of CRPC tumors is needed for innovative treatment strategies. In this review, we discuss the characteristics of CRPC tumors that lack AR activity and the temporal and spatial considerations for the conversion of an AR-dependent to an AR-independent tumor type. We describe the more prevalent treatment-emergent phenotypes arising in the CRPC disease continuum, including amphicrine, AR-low, double-negative, neuroendocrine and small cell phenotypes. We discuss the association between the loss of AR activity and tumor plasticity with a focus on the roles of transcription factors like SOX2, DNA methylation, alternative splicing, and the activity of epigenetic modifiers like EZH2, BRD4, LSD1, and the nBAF complex in conversion to a neuroendocrine or small cell phenotype in CRPC. We hypothesize that only a subset of CRPC tumors have the propensity for tumor plasticity and conversion to the neuroendocrine phenotype and outline how we might target these plastic and emergent phenotypes in CRPC. In conclusion, we assess the current and future avenues for treatment and determine that the heterogeneity of CRPCs lacking AR activity will require diverse treatment approaches. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
13510088
Volume :
28
Issue :
8
Database :
Complementary Index
Journal :
Endocrine-Related Cancer
Publication Type :
Academic Journal
Accession number :
151580348
Full Text :
https://doi.org/10.1530/ERC-21-0002