The Role of Non-Catalytic Domains of Hrp3 in Nucleosome Remodeling

The Helicase-related protein 3 (Hrp3), an ATP-dependent chromatin remodeling enzyme from the CHD family, is crucial for maintaining global nucleosome occupancy in <i>Schizosaccharomyces pombe</i> (<i>S. pombe)</i>. Although the ATPase domain of Hrp3 is essential for chromatin...

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Main Authors: Wenbo Dong, Punit Prasad, Andreas Lennartsson, Karl Ekwall
Format: Article
Language:English
Published: MDPI AG 2021-02-01
Series:International Journal of Molecular Sciences
Subjects:
Online Access:https://www.mdpi.com/1422-0067/22/4/1793
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spelling doaj-436cfeda0457474c8cd2f0063ed163302021-02-12T00:03:33ZengMDPI AGInternational Journal of Molecular Sciences1661-65961422-00672021-02-01221793179310.3390/ijms22041793The Role of Non-Catalytic Domains of Hrp3 in Nucleosome RemodelingWenbo Dong0Punit Prasad1Andreas Lennartsson2Karl Ekwall3Department of Biosciences and Nutrition, Karolinska Institutet NEO, 141 83 Huddinge, SwedenCancer Biology group, Institute of Life Sciences, NALCO Square, Bhubaneswar, Odhisa 751023, IndiaDepartment of Biosciences and Nutrition, Karolinska Institutet NEO, 141 83 Huddinge, SwedenDepartment of Biosciences and Nutrition, Karolinska Institutet NEO, 141 83 Huddinge, SwedenThe Helicase-related protein 3 (Hrp3), an ATP-dependent chromatin remodeling enzyme from the CHD family, is crucial for maintaining global nucleosome occupancy in <i>Schizosaccharomyces pombe</i> (<i>S. pombe)</i>. Although the ATPase domain of Hrp3 is essential for chromatin remodeling, the contribution of non-ATPase domains of Hrp3 is still unclear. Here, we investigated the role of non-ATPase domains using in vitro methods. In our study, we expressed and purified recombinant <i>S. pombe</i> histone proteins, reconstituted them into histone octamers, and assembled nucleosome core particles. Using reconstituted nucleosomes and affinity-purified wild type and mutant Hrp3 from <i>S. pombe</i> we created a homogeneous in vitro system to evaluate the ATP hydrolyzing capacity of truncated Hrp3 proteins. We found that all non-ATPase domain deletions (∆chromo, ∆SANT, ∆SLIDE, and ∆coupling region) lead to reduced ATP hydrolyzing activities in vitro with DNA or nucleosome substrates. Only the coupling region deletion showed moderate stimulation of ATPase activity with the nucleosome. Interestingly, affinity-purified Hrp3 showed co-purification with all core histones suggesting a strong association with the nucleosomes in vivo. However, affinity-purified Hrp3 mutant with SANT and coupling regions deletion showed complete loss of interactions with the nucleosomes, while SLIDE and chromodomain deletions reduced Hrp3 interactions with the nucleosomes. Taken together, nucleosome association and ATPase stimulation by DNA or nucleosomes substrate suggest that the enzymatic activity of Hrp3 is fine-tuned by unique contributions of all four non-catalytic domains.https://www.mdpi.com/1422-0067/22/4/1793<i>S. pombe</i> nucleosomesHrp3chromatin remodelingATPase activity
collection DOAJ
language English
format Article
sources DOAJ
author Wenbo Dong
Punit Prasad
Andreas Lennartsson
Karl Ekwall
spellingShingle Wenbo Dong
Punit Prasad
Andreas Lennartsson
Karl Ekwall
The Role of Non-Catalytic Domains of Hrp3 in Nucleosome Remodeling
International Journal of Molecular Sciences
<i>S. pombe</i> nucleosomes
Hrp3
chromatin remodeling
ATPase activity
author_facet Wenbo Dong
Punit Prasad
Andreas Lennartsson
Karl Ekwall
author_sort Wenbo Dong
title The Role of Non-Catalytic Domains of Hrp3 in Nucleosome Remodeling
title_short The Role of Non-Catalytic Domains of Hrp3 in Nucleosome Remodeling
title_full The Role of Non-Catalytic Domains of Hrp3 in Nucleosome Remodeling
title_fullStr The Role of Non-Catalytic Domains of Hrp3 in Nucleosome Remodeling
title_full_unstemmed The Role of Non-Catalytic Domains of Hrp3 in Nucleosome Remodeling
title_sort role of non-catalytic domains of hrp3 in nucleosome remodeling
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1661-6596
1422-0067
publishDate 2021-02-01
description The Helicase-related protein 3 (Hrp3), an ATP-dependent chromatin remodeling enzyme from the CHD family, is crucial for maintaining global nucleosome occupancy in <i>Schizosaccharomyces pombe</i> (<i>S. pombe)</i>. Although the ATPase domain of Hrp3 is essential for chromatin remodeling, the contribution of non-ATPase domains of Hrp3 is still unclear. Here, we investigated the role of non-ATPase domains using in vitro methods. In our study, we expressed and purified recombinant <i>S. pombe</i> histone proteins, reconstituted them into histone octamers, and assembled nucleosome core particles. Using reconstituted nucleosomes and affinity-purified wild type and mutant Hrp3 from <i>S. pombe</i> we created a homogeneous in vitro system to evaluate the ATP hydrolyzing capacity of truncated Hrp3 proteins. We found that all non-ATPase domain deletions (∆chromo, ∆SANT, ∆SLIDE, and ∆coupling region) lead to reduced ATP hydrolyzing activities in vitro with DNA or nucleosome substrates. Only the coupling region deletion showed moderate stimulation of ATPase activity with the nucleosome. Interestingly, affinity-purified Hrp3 showed co-purification with all core histones suggesting a strong association with the nucleosomes in vivo. However, affinity-purified Hrp3 mutant with SANT and coupling regions deletion showed complete loss of interactions with the nucleosomes, while SLIDE and chromodomain deletions reduced Hrp3 interactions with the nucleosomes. Taken together, nucleosome association and ATPase stimulation by DNA or nucleosomes substrate suggest that the enzymatic activity of Hrp3 is fine-tuned by unique contributions of all four non-catalytic domains.
topic <i>S. pombe</i> nucleosomes
Hrp3
chromatin remodeling
ATPase activity
url https://www.mdpi.com/1422-0067/22/4/1793
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