| Literature DB >> 31886609 |
Wenjie Liu1,2, Elisheva Biton3, Anjali Pathania3, Avi Matityahu3, Joseph Irudayaraj1,2, Itay Onn3.
Abstract
The cohesin complex plays an important role in the maintenance of genome stability. Cohesin is composed of four core subunits and a set of regulatory subunits that interact with the core subunits. Less is known about cohesin dynamics in live cells and on the contribution of individual subunits to the overall complex. Understanding the tethering mechanism of cohesin is still a challenge, especially because the proposed mechanisms are still not conclusive. Models proposed to describe tethering depend on either the monomeric cohesin ring or a cohesin dimer. Here, we investigate the role of cohesin dynamics and stoichiometry in live yeast cells at single-molecule resolution. We explore the effect of regulatory subunit deletion on cohesin mobility and found that depletion of different regulatory subunits has opposing effects. Finally, we show that cohesin exists mostly as a canonical monomer throughout the cell cycle, and its monomeric form is independent of its regulatory factors. Our results demonstrate that single-molecule tools have the potential to provide new insights into the cohesin mechanism of action in live cells.Entities:
Keywords: SMC complexes; chromosome; cohesin; fluorescence correlation spectroscopy; photon counting histogram
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Year: 2019 PMID: 31886609 PMCID: PMC7001500 DOI: 10.15252/embr.201948211
Source DB: PubMed Journal: EMBO Rep ISSN: 1469-221X Impact factor: 8.807