AI Article Synopsis

  • Chromatin, which is the material that DNA is made of, moves around in different ways that can affect how our genes work, especially when DNA gets damaged.
  • In yeast, when there are breaks in DNA, chromatin spreads out more, but in more complex organisms (like humans), it's more complicated.
  • When DNA is damaged, the movement of chromatin changes; it slows down far from the damage but moves more freely near the break, which helps the cell to repair the damage and avoid problems with DNA structure.

Article Abstract

Chromatin motions depend on and may regulate genome functions, in particular the DNA damage response. In yeast, DNA double-strand breaks (DSBs) globally increase chromatin diffusion, whereas in higher eukaryotes the impact of DSBs on chromatin dynamics is more nuanced. We mapped the motions of chromatin microdomains in mammalian cells using diffractive optics and photoactivatable chromatin probes and found a high level of spatial heterogeneity. DNA damage reduces heterogeneity and imposes spatially defined shifts in motions: Distal to DNA breaks, chromatin motions are globally reduced, whereas chromatin retains higher mobility at break sites. These effects are driven by context-dependent changes in chromatin compaction. Photoactivated lattices of chromatin microdomains are ideal to quantify microscale coupling of chromatin motion. We measured correlation distances up to 2 µm in the cell nucleus, spanning chromosome territories, and speculate that this correlation distance between chromatin microdomains corresponds to the physical separation of A and B compartments identified in chromosome conformation capture experiments. After DNA damage, chromatin motions become less correlated, a phenomenon driven by phase separation at DSBs. Our data indicate tight spatial control of chromatin motions after genomic insults, which may facilitate repair at the break sites and prevent deleterious contacts of DSBs, thereby reducing the risk of genomic rearrangements.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9304018PMC
http://dx.doi.org/10.1073/pnas.2205166119DOI Listing

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