TY - JOUR
T1 - Aneuploidy renders cancer cells vulnerable to mitotic checkpoint inhibition
AU - Cohen-Sharir, Yael
AU - McFarland, James M.
AU - Abdusamad, Mai
AU - Marquis, Carolyn
AU - Bernhard, Sara V.
AU - Kazachkova, Mariya
AU - Tang, Helen
AU - Ippolito, Marica R.
AU - Laue, Kathrin
AU - Zerbib, Johanna
AU - Malaby, Heidi L.H.
AU - Jones, Andrew
AU - Stautmeister, Lisa Marie
AU - Bockaj, Irena
AU - Wardenaar, René
AU - Lyons, Nicholas
AU - Nagaraja, Ankur
AU - Bass, Adam J.
AU - Spierings, Diana C.J.
AU - Foijer, Floris
AU - Beroukhim, Rameen
AU - Santaguida, Stefano
AU - Golub, Todd R.
AU - Stumpff, Jason
AU - Storchová, Zuzana
AU - Ben-David, Uri
N1 - Publisher Copyright: © 2021, The Author(s), under exclusive licence to Springer Nature Limited.
PY - 2021/2/18
Y1 - 2021/2/18
N2 - Selective targeting of aneuploid cells is an attractive strategy for cancer treatment1. However, it is unclear whether aneuploidy generates any clinically relevant vulnerabilities in cancer cells. Here we mapped the aneuploidy landscapes of about 1,000 human cancer cell lines, and analysed genetic and chemical perturbation screens2–9 to identify cellular vulnerabilities associated with aneuploidy. We found that aneuploid cancer cells show increased sensitivity to genetic perturbation of core components of the spindle assembly checkpoint (SAC), which ensures the proper segregation of chromosomes during mitosis10. Unexpectedly, we also found that aneuploid cancer cells were less sensitive than diploid cells to short-term exposure to multiple SAC inhibitors. Indeed, aneuploid cancer cells became increasingly sensitive to inhibition of SAC over time. Aneuploid cells exhibited aberrant spindle geometry and dynamics, and kept dividing when the SAC was inhibited, resulting in the accumulation of mitotic defects, and in unstable and less-fit karyotypes. Therefore, although aneuploid cancer cells could overcome inhibition of SAC more readily than diploid cells, their long-term proliferation was jeopardized. We identified a specific mitotic kinesin, KIF18A, whose activity was perturbed in aneuploid cancer cells. Aneuploid cancer cells were particularly vulnerable to depletion of KIF18A, and KIF18A overexpression restored their response to SAC inhibition. Our results identify a therapeutically relevant, synthetic lethal interaction between aneuploidy and the SAC.
AB - Selective targeting of aneuploid cells is an attractive strategy for cancer treatment1. However, it is unclear whether aneuploidy generates any clinically relevant vulnerabilities in cancer cells. Here we mapped the aneuploidy landscapes of about 1,000 human cancer cell lines, and analysed genetic and chemical perturbation screens2–9 to identify cellular vulnerabilities associated with aneuploidy. We found that aneuploid cancer cells show increased sensitivity to genetic perturbation of core components of the spindle assembly checkpoint (SAC), which ensures the proper segregation of chromosomes during mitosis10. Unexpectedly, we also found that aneuploid cancer cells were less sensitive than diploid cells to short-term exposure to multiple SAC inhibitors. Indeed, aneuploid cancer cells became increasingly sensitive to inhibition of SAC over time. Aneuploid cells exhibited aberrant spindle geometry and dynamics, and kept dividing when the SAC was inhibited, resulting in the accumulation of mitotic defects, and in unstable and less-fit karyotypes. Therefore, although aneuploid cancer cells could overcome inhibition of SAC more readily than diploid cells, their long-term proliferation was jeopardized. We identified a specific mitotic kinesin, KIF18A, whose activity was perturbed in aneuploid cancer cells. Aneuploid cancer cells were particularly vulnerable to depletion of KIF18A, and KIF18A overexpression restored their response to SAC inhibition. Our results identify a therapeutically relevant, synthetic lethal interaction between aneuploidy and the SAC.
UR - http://www.scopus.com/inward/record.url?scp=85099962464&partnerID=8YFLogxK
U2 - https://doi.org/10.1038/s41586-020-03114-6
DO - https://doi.org/10.1038/s41586-020-03114-6
M3 - مقالة
C2 - 33505028
SN - 0028-0836
VL - 590
SP - 486
EP - 491
JO - Nature
JF - Nature
IS - 7846
ER -