The Energetics and Physiological Impact of Cohesin Extrusion
Author(s) -
Laura Vian,
Aleksandra Pękowska,
Suhas S.P. Rao,
Kyong-Rim Kieffer-Kwon,
Seolkyoung Jung,
Laura Baranello,
SuChen Huang,
Laïla El Khattabi,
Marei Dose,
Nathanael Pruett,
Adrian L. Sanborn,
Andrés Canela,
Yaakov Maman,
Anna Oksanen,
Wolfgang Resch,
Xingwang Li,
Byoungkoo Lee,
Alexander L. Kovalchuk,
Zhonghui Tang,
Steevenson Nelson,
Michele Di Pierro,
Ryan R. Cheng,
Ido Machol,
Brian Glenn St Hilaire,
Neva C. Durand,
Muhammad S. Shamim,
Elena K. Stamenova,
José N. Onuchic,
Yijun Ruan,
André Nussenzweig,
David Levens,
E Aiden,
Rafael Casellas
Publication year - 2018
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2018.03.072
Subject(s) - biology , energetics , cohesin , extrusion , microbiology and biotechnology , evolutionary biology , genetics , ecology , gene , meiosis , materials science , metallurgy
Cohesin extrusion is thought to play a central role in establishing the architecture of mammalian genomes. However, extrusion has not been visualized in vivo, and thus, its functional impact and energetics are unknown. Using ultra-deep Hi-C, we show that loop domains form by a process that requires cohesin ATPases. Once formed, however, loops and compartments are maintained for hours without energy input. Strikingly, without ATP, we observe the emergence of hundreds of CTCF-independent loops that link regulatory DNA. We also identify architectural "stripes," where a loop anchor interacts with entire domains at high frequency. Stripes often tether super-enhancers to cognate promoters, and in B cells, they facilitate Igh transcription and recombination. Stripe anchors represent major hotspots for topoisomerase-mediated lesions, which promote chromosomal translocations and cancer. In plasmacytomas, stripes can deregulate Igh-translocated oncogenes. We propose that higher organisms have coopted cohesin extrusion to enhance transcription and recombination, with implications for tumor development.
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