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Acquisition of chromosome instability is a mechanism to evade oncogene addiction.


ABSTRACT: Chromosome instability (CIN) has been associated with therapeutic resistance in many cancers. However, whether tumours become genomically unstable as an evolutionary mechanism to overcome the bottleneck exerted by therapy is not clear. Using a CIN model of Kras-driven breast cancer, we demonstrate that aneuploid tumours acquire genetic modifications that facilitate the development of resistance to targeted therapy faster than euploid tumours. We further show that the few initially chromosomally stable cancers that manage to persist during treatment do so concomitantly with the acquisition of CIN. Whole-genome sequencing analysis revealed that the most predominant genetic alteration in resistant tumours, originated from either euploid or aneuploid primary tumours, was an amplification on chromosome 6 containing the cMet oncogene. We further show that these tumours are dependent on cMet since its pharmacological inhibition leads to reduced growth and increased cell death. Our results highlight that irrespective of the initial CIN levels, cancer genomes are dynamic and the acquisition of a certain level of CIN, either induced or spontaneous, is a mechanism to circumvent oncogene addiction.

SUBMITTER: Salgueiro L 

PROVIDER: S-EPMC7059010 | biostudies-literature | 2020 Mar

REPOSITORIES: biostudies-literature

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Acquisition of chromosome instability is a mechanism to evade oncogene addiction.

Salgueiro Lorena L   Buccitelli Christopher C   Rowald Konstantina K   Somogyi Kalman K   Kandala Sridhar S   Korbel Jan O JO   Sotillo Rocio R  

EMBO molecular medicine 20200206 3


Chromosome instability (CIN) has been associated with therapeutic resistance in many cancers. However, whether tumours become genomically unstable as an evolutionary mechanism to overcome the bottleneck exerted by therapy is not clear. Using a CIN model of Kras-driven breast cancer, we demonstrate that aneuploid tumours acquire genetic modifications that facilitate the development of resistance to targeted therapy faster than euploid tumours. We further show that the few initially chromosomally  ...[more]

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