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Replicative Instability Drives Cancer Progression

Authors :: Benjamin B. Morris
Jason P. Smith
Qi Zhang
Zhijie Jiang
Oliver A. Hampton
Michelle L. Churchman
Susanne M. Arnold
Dwight H. Owen
Jhanelle E. Gray
Patrick M. Dillon
Hatem H. Soliman
Daniel G. Stover
Howard Colman
Arnab Chakravarti
Kenneth H. Shain
Ariosto S. Silva
John L. Villano
Michael A. Vogelbaum
Virginia F. Borges
Wallace L. Akerley
Ryan D. Gentzler
Richard D. Hall
Cindy B. Matsen
C. M. Ulrich
Andrew R. Post
David A. Nix
Eric A. Singer
James M. Larner
Peter Todd Stukenberg
David R. Jones
Marty W. Mayo
Source :: Biomolecules, Vol 12, Iss 11, p 1570 (2022)
Publication Year :: 2022
Publisher :: MDPI AG, 2022.
Abstract: In the past decade, defective DNA repair has been increasingly linked with cancer progression. Human tumors with markers of defective DNA repair and increased replication stress exhibit genomic instability and poor survival rates across tumor types. Seminal studies have demonstrated that genomic instability develops following inactivation of BRCA1, BRCA2, or BRCA-related genes. However, it is recognized that many tumors exhibit genomic instability but lack BRCA inactivation. We sought to identify a pan-cancer mechanism that underpins genomic instability and cancer progression in BRCA-wildtype tumors. Methods: Using multi-omics data from two independent consortia, we analyzed data from dozens of tumor types to identify patient cohorts characterized by poor outcomes, genomic instability, and wildtype BRCA genes. We developed several novel metrics to identify the genetic underpinnings of genomic instability in tumors with wildtype BRCA. Associated clinical data was mined to analyze patient responses to standard of care therapies and potential differences in metastatic dissemination. Results: Systematic analysis of the DNA repair landscape revealed that defective single-strand break repair, translesion synthesis, and non-homologous end-joining effectors drive genomic instability in tumors with wildtype BRCA and BRCA-related genes. Importantly, we find that loss of these effectors promotes replication stress, therapy resistance, and increased primary carcinoma to brain metastasis. Conclusions: Our results have defined a new pan-cancer class of tumors characterized by replicative instability (RIN). RIN is defined by the accumulation of intra-chromosomal, gene-level gain and loss events at replication stress sensitive (RSS) genome sites. We find that RIN accelerates cancer progression by driving copy number alterations and transcriptional program rewiring that promote tumor evolution. Clinically, we find that RIN drives therapy resistance and distant metastases across multiple tumor types.