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The Arp8 and Arp4 module acts as a DNA sensor controlling INO80 chromatin remodeling

Sandipan Brahma, Mzwanele Ngubo, Somnath Paul, Maheshi Udugama and Blaine Bartholomew ()
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Sandipan Brahma: The University of Texas MD Anderson Cancer Center
Mzwanele Ngubo: The University of Texas MD Anderson Cancer Center
Somnath Paul: The University of Texas MD Anderson Cancer Center
Maheshi Udugama: Southern Illinois University
Blaine Bartholomew: The University of Texas MD Anderson Cancer Center

Nature Communications, 2018, vol. 9, issue 1, 1-10

Abstract: Abstract Nuclear actin and actin-related proteins (Arps) are key components of chromatin remodeling and modifying complexes. Although Arps are essential for the functions of chromatin remodelers, their specific roles and mechanisms are unclear. Here we define the nucleosome binding interfaces and functions of the evolutionarily conserved Arps in the yeast INO80 chromatin remodeling complex. We show that the N-terminus of Arp8, C-terminus of Arp4 and the HSA domain of Ino80 bind extranucleosomal DNA 37–51 base pairs from the edge of nucleosomes and function as a DNA-length sensor that regulates nucleosome sliding by INO80. Disruption of Arp8 and Arp4 binding to DNA uncouples ATP hydrolysis from nucleosome mobilization by disengaging Arp5 from the acidic patch on histone H2A-H2B and the Ino80-ATPase domain from the Super-helical Location (SHL) -6 of nucleosomes. Our data suggest a functional interplay between INO80’s Arp8-Arp4-actin and Arp5 modules in sensing the DNA length separating nucleosomes and regulating nucleosome positioning.

Date: 2018
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DOI: 10.1038/s41467-018-05710-7

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