Chromosomal Instability Confers Intrinsic Multidrug Resistance
Alvin J.X. Lee,David Endesfelder,Andrew Rowan,Axel Walther,Nicolai Juul Birkbak,P. Andrew Futreal,Julian Downward,Zoltan Szallasi,Zoltan Szallasi,Ian Tomlinson,Michael Howell,Maik Kschischo,Charles Swanton +12 more
TL;DR: The results suggest that stratifying tumor responses according to CINstatus should be considered within the context of clinical trials to minimize the confounding effects of tumor CIN status on drug sensitivity.
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Abstract: Aneuploidy is associated with poor prognosis in solid tumors. Spontaneous chromosome missegregation events in aneuploid cells promote chromosomal instability (CIN) that may contribute to the acquisition of multidrug resistance in vitro and heighten risk for tumor relapse in animal models. Identification of distinct therapeutic agents that target tumor karyotypic complexity has important clinical implications. To identify distinct therapeutic approaches to specifically limit the growth of CIN tumors, we focused on a panel of colorectal cancer (CRC) cell lines, previously classified as either chromosomally unstable (CIN(+)) or diploid/near-diploid (CIN(-)), and treated them individually with a library of kinase inhibitors targeting components of signal transduction, cell cycle, and transmembrane receptor signaling pathways. CIN(+) cell lines displayed significant intrinsic multidrug resistance compared with CIN(-) cancer cell lines, and this seemed to be independent of somatic mutation status and proliferation rate. Confirming the association of CIN rather than ploidy status with multidrug resistance, tetraploid isogenic cells that had arisen from diploid cell lines displayed lower drug sensitivity than their diploid parental cells only with increasing chromosomal heterogeneity and isogenic cell line models of CIN(+) displayed multidrug resistance relative to their CIN(-) parental cancer cell line derivatives. In a meta-analysis of CRC outcome following cytotoxic treatment, CIN(+) predicted worse progression-free or disease-free survival relative to patients with CIN(-) disease. Our results suggest that stratifying tumor responses according to CIN status should be considered within the context of clinical trials to minimize the confounding effects of tumor CIN status on drug sensitivity.
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Citations
APC/C Dysfunction Limits Excessive Cancer Chromosomal Instability.
Laurent Sansregret,James O. Patterson,Sally M. Dewhurst,Carlos López-García,Andre Koch,Nicholas McGranahan,William C. H. Chao,David J. Barry,Andrew Rowan,Rachael Instrell,Stuart Horswell,Michael Way,Michael Howell,Martin R. Singleton,René H. Medema,Paul Nurse,Mark Petronczki,Mark Petronczki,Charles Swanton +18 more
TL;DR: A mechanism whereby cancers balance the evolutionary advantages associated with CIN against the fitness costs caused by excessive genome instability is reported, providing insight into the consequence of CDC27 APC/C subunit driver mutations in cancer.
Genomic instability, inflammatory signaling and response to cancer immunotherapy.
TL;DR: A review of inflammatory signaling pathways induced by various sources of genomic instability, adaptation mechanisms that suppress inflammatory signaling, and implications for cancer immunotherapy are presented in this article, where inflammatory signaling has pleiotropic effects, including enhanced anti-tumor immunity and potentially results in sensitization of cancer cells to immune checkpoint inhibitors.
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DNA copy number changes define spatial patterns of heterogeneity in colorectal cancer
Soulafa Mamlouk,Soulafa Mamlouk,Liam Harold Childs,Daniela Aust,Daniel Heim,Friederike Melching,Cristiano Oliveira,Thomas Wolf,Pawel Durek,Dirk Schumacher,Dirk Schumacher,Hendrik Bläker,Moritz von Winterfeld,Bastian Gastl,Kerstin Möhr,Andrea Menne,Andrea Menne,Silke Zeugner,Torben Redmer,Torben Redmer,Dido Lenze,Sascha Tierling,Markus Möbs,Wilko Weichert,Gunnar Folprecht,Eric Blanc,Dieter Beule,Reinhold Schäfer,Reinhold Schäfer,Markus Morkel,Frederick Klauschen,Ulf Leser,Christine Sers +32 more
TL;DR: Analysis of DNA sequence and DNA copy-number heterogeneity in colorectal cancer by targeted high-depth sequencing of 100 most frequently altered genes identifies evenly distributed coding mutations in APC and TP53 in all tumour areas, yet highly variable gene copy numbers in numerous genes.
Genetic instability: tipping the balance.
Aniek Janssen,René H. Medema +1 more
TL;DR: The mechanisms that can cause gross chromosomal aberrations, and how these affect tumor cell viability are reviewed.
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A Double-Edged Sword: How Oncogenes and Tumor Suppressor Genes Can Contribute to Chromosomal Instability
Bernardo Orr,Duane A. Compton +1 more
TL;DR: The results indicate that the induction of CIN can no longer be considered separately from the cancer-associated driver mutations and how the oncogenic activation of key signal transduction pathways contributes to the inductionof CIN is discussed.
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