Subtype Heterogeneity and Epigenetic Convergence in Neuroendocrine Prostate Cancer

Paloma Cejas
Yingtian Xie
Alba Font-Tello
Klothilda Lim
Sudeepa Syamala
Xintao Qiu
Alok K. Tewari
Neel Shah
Holly M Nguyen
Radhika A. Patel
Lisha Brown
Ilsa Coleman
Wenzel M. Hackeng
Lodewijk Brosens
Koen M.A. Dreijerink
Leigh Ellis
Sarah Abou Alaiwi
Ji-Heui Seo
Mark Pomerantz
Alessandra Dall’Agnese
Jett Crowdis
Eliezer M. Van Allen
Joaquim Bellmunt
Colm Morrisey
Peter S. Nelson
James DeCaprio
Anna Farago
Nicholas Dyson
Benjamin Drapkin
X. Shirley Liu
Matthew Freedman
Michael C. Haffner
Eva Corey
Myles Brown
Henry W. Long

2 evaluations Published on Sep 14, 2020

This article on Sciety

Abstract

Neuroendocrine carcinomas (NEC) are tumors expressing markers of neuronal differentiation that can arise at different anatomic sites but have strong histological and clinical similarities. Here we report the chromatin landscapes of a range of human NECs and show convergence to the activation of a common epigenetic program. With a particular focus on treatment emergent neuroendocrine prostate cancer (NEPC), we analyzed cell lines, patient-derived xenograft (PDX) models and human clinical samples to show the existence of two distinct NEPC subtypes based on the expression of the neuronal transcription factors ASCL1 and NEUROD1. While in cell lines and PDX models these subtypes are mutually exclusive, single cell analysis of human clinical samples exhibit a more complex tumor structure with subtypes coexisting as separate sub-populations within the same tumor. These tumor sub-populations differ genetically and epigenetically contributing to intra- and inter-tumoral heterogeneity in human metastases. Overall our results provide a deeper understanding of the shared clinicopathological characteristics shown by NECs. Furthermore, the intratumoral heterogeneity of human NEPCs suggests the requirement of simultaneous targeting of coexisting tumor populations as a therapeutic strategy.

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