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Integrated analyses highlight interactions between the three-dimensional genome and DNA, RNA and epigenomic alterations in metastatic prostate cancer.

Shuang G Zhao ,
Matthew Bootsma ,
Stanley Zhou ,
Raunak Shrestha ,
Thaidy Moreno-Rodriguez ,
Arian Lundberg ,
Chu Pan ,
Christopher Arlidge ,
James R Hawley ,
Adam Foye ,
Alana S Weinstein ,
Martin Sjöström ,
Meng Zhang ,
Haolong Li ,
Lisa N Chesner ,
Nicholas R Rydzewski ,
Kyle T Helzer ,
Yue Shi ,
,
Molly Lynch ,
Scott M Dehm ,
Joshua M Lang ,
Joshi J Alumkal ,
Hansen H He ,
Alexander W Wyatt ,
Rahul Aggarwal ,
Wilbert Zwart ,
Eric J Small ,
David A Quigley ,
Mathieu Lupien ,
Felix Y Feng

Abstract

The impact of variations in the three-dimensional structure of the genome has been recognized, but solid cancer tissue studies are limited. Here, we performed integrated deep Hi-C sequencing with matched whole-genome sequencing, whole-genome bisulfite sequencing, 5-hydroxymethylcytosine (5hmC) sequencing and RNA sequencing across a cohort of 80 biopsy samples from patients with metastatic castration-resistant prostate cancer. Dramatic differences were present in gene expression, 5-methylcytosine/5hmC methylation and in structural variation versus mutation rate between A and B (open and closed) chromatin compartments. A subset of tumors exhibited depleted regional chromatin contacts at the AR locus, linked to extrachromosomal circular DNA (ecDNA) and worse response to AR signaling inhibitors. We also identified topological subtypes associated with stark differences in methylation structure, gene expression and prognosis. Our data suggested that DNA interactions may predispose to structural variant formation, exemplified by the recurrent TMPRSS2-ERG fusion. This comprehensive integrated sequencing effort represents a unique clinical tumor resource.

More about this publication

Nature genetics

Volume 56
Issue nr. 8
Pages 1689-1700
Publication date 01-08-2024

Full text links

Publisher website (DOI) 10.1038/s41588-024-01826-3
Europe PubMed Central 39020220
Pubmed 39020220

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