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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Mitotic slippage: an old tale with a new twist
TL;DR: The rationale of targeting CEP55 in vivo could prove to be a novel and effective therapeutic strategy for sensitizing cells to microtubule inhibitors and might offer significantly improved patient outcome.
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Aneuploidy in health, disease, and aging.
TL;DR: In vivo studies of mouse models for the mitotic checkpoint protein BubR1 have uncovered important new insights into the extremely complex aneuploidy–cancer relationship but also into the molecular mechanisms underlying proper and aberrant chromosome segregation.
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Chromosomal instability accelerates the evolution of resistance to anti-cancer therapies
Devon A. Lukow,Erin L. Sausville,Pavit Suri,Narendra Kumar Chunduri,Justin Leu,Jude Kendall,Zihua Wang,Zuzana Storchova,Jason M. Sheltzer +8 more
TL;DR: While chromosomal instability generally antagonizes cell fitness, it also provides phenotypic plasticity to cancer cells that can allow them to adapt to diverse stressful environments and suggest that aneuploidy may function as an under-explored cause of therapy failure in human tumors.
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High level of chromosomal instability in circulating tumor cells of ROS1-rearranged non-small-cell lung cancer
Emma Pailler,Emma Pailler,Nathalie Auger,Colin R Lindsay,Colin R Lindsay,Philippe Vielh,Philippe Vielh,A Islas-Morris-Hernandez,Isabelle Borget,Maud Ngo-Camus,David Planchard,Jean-Charles Soria,Jean-Charles Soria,Benjamin Besse,Françoise Farace,Françoise Farace +15 more
TL;DR: ROS1-rearrangement can be detected in circulating tumor cells of ROS1- rearranged non-small-cell lung cancer patients, offering perspectives for diagnosing patients eligible for ROS 1-inhibitor therapy.
116
Non-cell-autonomous cancer progression from chromosomal instability
Jun Li,Melissa J. Hubisz,Ethan M. Earlie,Mercedes Duran,Christy Hong,Austin A Varela,Emanuele Lettera,Matthew Deyell,Bernardo Tavora,J. Havel,Su Myat Phyu,Amit Dipak Amin,Karolina Budre,Erina Kamiya,Julie-Ann Cavallo,Christopher Garris,Simon N. Powell,Jorge S. Reis-Filho,Hannah Y Wen,Sarah E. Bettigole,Atif J. Khan,Benjamin Izar,Eileen Parkes,Ashley M. Laughney,Samuel F. Bakhoum +24 more
TL;DR: It is shown that CIN and pervasive cGAS activation in micronuclei are associated with ER stress signalling, immune suppression and metastasis in human triple-negative breast cancer, highlighting a viable strategy to identify and therapeutically intervene in tumours spurred by CIN-induced inflammation.
112
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