Cohesin depleted cells rebuild functional nuclear compartments after endomitosis

Author:

Cremer MarionORCID,Brandstetter KatharinaORCID,Maiser AndreasORCID,Rao Suhas S. P.,Schmid Volker J.ORCID,Guirao-Ortiz MiguelORCID,Mitra Namita,Mamberti StefaniaORCID,Klein Kyle N.,Gilbert David M.ORCID,Leonhardt HeinrichORCID,Cardoso M. CristinaORCID,Aiden Erez Lieberman,Harz HartmannORCID,Cremer ThomasORCID

Abstract

AbstractCohesin plays an essential role in chromatin loop extrusion, but its impact on a compartmentalized nuclear architecture, linked to nuclear functions, is less well understood. Using live-cell and super-resolved 3D microscopy, here we find that cohesin depletion in a human colon cancer derived cell line results in endomitosis and a single multilobulated nucleus with chromosome territories pervaded by interchromatin channels. Chromosome territories contain chromatin domain clusters with a zonal organization of repressed chromatin domains in the interior and transcriptionally competent domains located at the periphery. These clusters form microscopically defined, active and inactive compartments, which likely correspond to A/B compartments, which are detected with ensemble Hi-C. Splicing speckles are observed nearby within the lining channel system. We further observe that the multilobulated nuclei, despite continuous absence of cohesin, pass through S-phase with typical spatio-temporal patterns of replication domains. Evidence for structural changes of these domains compared to controls suggests that cohesin is required for their full integrity.

Funder

Deutsche Forschungsgemeinschaft

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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