Confinement plus Myosin-II suppression maximizes heritable loss of chromosomes, as revealed by live-cell ChReporters

A cell's mechanical environment can have many effects, but whether it impacts a cell's DNA sequence has remained unclear. To investigate this, we developed a live-cell method to measure changes in chromosome numbers. We edited constitutive genes with GFP/RFP-tags on single alleles and disc...

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Veröffentlicht in:Journal of cell science 2023-06, Vol.136 (11)
Hauptverfasser: Hayes, Brandon H, Zhu, Peter Kuangzheng, Wang, Mai, Pfeifer, Charlotte R, Xia, Yuntao, Phan, Steven, Andrechak, Jason C, Du, Junhong, Tobin, Michael P, Anlas, Alisya, Dooling, Lawrence J, Vashisth, Manasvita, Irianto, Jerome, Lampson, Michael A, Discher, Dennis E
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Sprache:eng
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Zusammenfassung:A cell's mechanical environment can have many effects, but whether it impacts a cell's DNA sequence has remained unclear. To investigate this, we developed a live-cell method to measure changes in chromosome numbers. We edited constitutive genes with GFP/RFP-tags on single alleles and discovered that cells that lose Chromosome-reporters (ChReporters) become non-fluorescent. We applied our new tools to confined mitosis and to inhibition of the putative tumor suppressor Myosin-II. We quantified compression of mitotic chromatin in vivo and demonstrated that similar compression in vitro resulted in cell death, but also rare and heritable ChReptorter loss. Myosin-II suppression rescued lethal multipolar divisions and maximized ChReporter loss in 3D-compression and 2D-confinement, but not in standard 2D-culture. ChReporter loss associated with chromosome mis-segregation, rather than just the number of divisions, and loss in vitro and in mice was selected against in subsequent 2D-cultures. Inhibition of the spindle assembly checkpoint (SAC) caused ChReporter loss in 2D, as expected, but not in 3D-compression, suggesting a SAC perturbation. Thus, confinement and myosin-II affect DNA sequence and mechano-evolution, and ChReporters enable diverse studies of viable genetic changes.
ISSN:0021-9533
1477-9137
1477-9137
DOI:10.1242/jcs.260753