Whole-genome Doubling Confers Unique Genetic Vulnerabilities on Tumour Cells

Overview

Journal Nature

Specialty Science

Date 2021 Jan 28

PMID 33505027

Citations 113

Authors

Ryan J Quinton

Amanda DiDomizio

Marc A Vittoria

Kristyna Kotynkova

Carlos J Ticas

Sheena Patel

Yusuke Koga

Jasmine Vakhshoorzadeh

Nicole Hermance

Taruho S Kuroda

Neha Parulekar

Alison M Taylor

Amity L Manning

Joshua D Campbell

Neil J Ganem

Affiliations

Soon will be listed here.

Abstract

Whole-genome doubling (WGD) is common in human cancers, occurring early in tumorigenesis and generating genetically unstable tetraploid cells that fuel tumour development. Cells that undergo WGD (WGD cells) must adapt to accommodate their abnormal tetraploid state; however, the nature of these adaptations, and whether they confer vulnerabilities that can be exploited therapeutically, is unclear. Here, using sequencing data from roughly 10,000 primary human cancer samples and essentiality data from approximately 600 cancer cell lines, we show that WGD gives rise to common genetic traits that are accompanied by unique vulnerabilities. We reveal that WGD cells are more dependent than WGD cells on signalling from the spindle-assembly checkpoint, DNA-replication factors and proteasome function. We also identify KIF18A, which encodes a mitotic kinesin protein, as being specifically required for the viability of WGD cells. Although KIF18A is largely dispensable for accurate chromosome segregation during mitosis in WGD cells, its loss induces notable mitotic errors in WGD cells, ultimately impairing cell viability. Collectively, our results suggest new strategies for specifically targeting WGD cancer cells while sparing the normal, non-transformed WGD cells that comprise human tissue.

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