Dynamic Organization of Chromatin Domains Revealed by Super-Resolution Live-Cell Imaging.

Mol Cell

Biological Macromolecules Laboratory, Structural Biology Center, National Institute of Genetics, Mishima, Shizuoka 411-8540, Japan; Department of Genetics, School of Life Science, Sokendai (Graduate University for Advanced Studies), Mishima, Shizuoka 411-8540, Japan. Electronic address:

Published: July 2017

AI Article Synopsis

  • The eukaryotic genome is organized as chromatin, and its higher-order structures dynamically regulate gene expression and cellular processes, though their formation and behavior are not fully understood.
  • Researchers used advanced imaging techniques to observe how nucleosomes cluster into compact domains, which vary in movement based on factors like cell differentiation and chromatin composition.
  • Their findings suggest that these nucleosomal domains play a role in organizing chromosomes during cell division and may serve as functional units for genetic information throughout the cell cycle.

Article Abstract

The eukaryotic genome is organized within cells as chromatin. For proper information output, higher-order chromatin structures can be regulated dynamically. How such structures form and behave in various cellular processes remains unclear. Here, by combining super-resolution imaging (photoactivated localization microscopy [PALM]) and single-nucleosome tracking, we developed a nuclear imaging system to visualize the higher-order structures along with their dynamics in live mammalian cells. We demonstrated that nucleosomes form compact domains with a peak diameter of ∼160 nm and move coherently in live cells. The heterochromatin-rich regions showed more domains and less movement. With cell differentiation, the domains became more apparent, with reduced dynamics. Furthermore, various perturbation experiments indicated that they are organized by a combination of factors, including cohesin and nucleosome-nucleosome interactions. Notably, we observed the domains during mitosis, suggesting that they act as building blocks of chromosomes and may serve as information units throughout the cell cycle.

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Source
http://dx.doi.org/10.1016/j.molcel.2017.06.018DOI Listing

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