Flexible and dynamic nucleosome fiber in living mammalian cells.

Nucleus

Biological Macromolecules Laboratory; Structural Biology Center; National Institute of Genetics; Mishima, Japan; Institute for Advanced Biosciences; Keio University; Fujisawa, Japan; Laboratory for Biochemical Simulation; RIKEN Quantitative Biology Center; Suita, Japan; Cellular Informatics Laboratory; RIKEN; Wako, Japan; Cellular Dynamics Program; Marine Biological Laboratory; Woods Hole, MA USA; Department of Genetics; School of Life Science; Graduate University for Advanced Studies (Sokendai); Mishima, Japan; The Institute of Scientific and Industrial Research; Osaka University; Ibaraki, Japan.

Published: August 2014

AI Article Synopsis

  • Genomic DNA is structured as chromatin in a 3D form, allowing proteins to interact and carry out various cellular functions, although the exact mechanism of this interaction is still unclear.
  • Recent research, including cryomicroscopy and X-ray analyses, shows that chromatin is made of irregularly folded nucleosome fibers instead of a rigid 30-nm fiber, leading to a more dynamic and less constrained structure.
  • A combination of imaging techniques revealed that nucleosomes in living cells exhibit significant movement (about 50 nm every 30 ms) due to Brownian motion, suggesting that this dynamic behavior enhances chromatin accessibility for protein scanning of the genome.

Article Abstract

Genomic DNA is organized three dimensionally within cells as chromatin and is searched and read by various proteins by an unknown mechanism; this mediates diverse cell functions. Recently, several pieces of evidence, including our cryomicroscopy and synchrotron X-ray scattering analyses, have demonstrated that chromatin consists of irregularly folded nucleosome fibers without a 30-nm chromatin fiber (i.e., a polymer melt-like structure). This melt-like structure implies a less physically constrained and locally more dynamic state, which may be crucial for protein factors to scan genomic DNA. Using a combined approach of fluorescence correlation spectroscopy, Monte Carlo computer simulations, and single nucleosome imaging, we demonstrated the flexible and dynamic nature of the nucleosome fiber in living mammalian cells. We observed local nucleosome fluctuation (~50 nm movement/30 ms) caused by Brownian motion. Our in vivo/in silico results suggest that local nucleosome dynamics facilitate chromatin accessibility and play a critical role in the scanning of genome information.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3899123PMC
http://dx.doi.org/10.4161/nucl.26053DOI Listing

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