A capped Tudor domain within a core subunit of the Sin3L/Rpd3L histone deacetylase complex binds to nucleic acid G-quadruplexes

Chromatin-modifying complexes containing histone deacetylase (HDAC) activities play critical roles in the regulation of gene transcription in eukaryotes. These complexes are thought to lack intrinsic DNA-binding activity, but according to a well-established paradigm, they are recruited via protein–p...

Descripción completa

Detalles Bibliográficos
Autores principales: Marcum, Ryan Dale, Hsieh, Joseph, Giljen, Maksim, Justice, Emily, Daffern, Nicolas, Zhang, Yongbo, Radhakrishnan, Ishwar
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8800102/
https://www.ncbi.nlm.nih.gov/pubmed/34979096
http://dx.doi.org/10.1016/j.jbc.2021.101558
_version_ 1784642191568666624
author Marcum, Ryan Dale
Hsieh, Joseph
Giljen, Maksim
Justice, Emily
Daffern, Nicolas
Zhang, Yongbo
Radhakrishnan, Ishwar
author_facet Marcum, Ryan Dale
Hsieh, Joseph
Giljen, Maksim
Justice, Emily
Daffern, Nicolas
Zhang, Yongbo
Radhakrishnan, Ishwar
author_sort Marcum, Ryan Dale
collection PubMed
description Chromatin-modifying complexes containing histone deacetylase (HDAC) activities play critical roles in the regulation of gene transcription in eukaryotes. These complexes are thought to lack intrinsic DNA-binding activity, but according to a well-established paradigm, they are recruited via protein–protein interactions by gene-specific transcription factors and posttranslational histone modifications to their sites of action on the genome. The mammalian Sin3L/Rpd3L complex, comprising more than a dozen different polypeptides, is an ancient HDAC complex found in diverse eukaryotes. The subunits of this complex harbor conserved domains and motifs of unknown structure and function. Here, we show that Sds3, a constitutively-associated subunit critical for the proper functioning of the Sin3L/Rpd3L complex, harbors a type of Tudor domain that we designate the capped Tudor domain. Unlike canonical Tudor domains that bind modified histones, the Sds3 capped Tudor domain binds to nucleic acids that can form higher-order structures such as G-quadruplexes and shares similarities with the knotted Tudor domain of the Esa1 histone acetyltransferase that was previously shown to bind single-stranded RNA. Our findings expand the range of macromolecules capable of recruiting the Sin3L/Rpd3L complex and draw attention to potentially new biological roles for this HDAC complex.
format Online
Article
Text
id pubmed-8800102
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher American Society for Biochemistry and Molecular Biology
record_format MEDLINE/PubMed
spelling pubmed-88001022022-02-03 A capped Tudor domain within a core subunit of the Sin3L/Rpd3L histone deacetylase complex binds to nucleic acid G-quadruplexes Marcum, Ryan Dale Hsieh, Joseph Giljen, Maksim Justice, Emily Daffern, Nicolas Zhang, Yongbo Radhakrishnan, Ishwar J Biol Chem Research Article Chromatin-modifying complexes containing histone deacetylase (HDAC) activities play critical roles in the regulation of gene transcription in eukaryotes. These complexes are thought to lack intrinsic DNA-binding activity, but according to a well-established paradigm, they are recruited via protein–protein interactions by gene-specific transcription factors and posttranslational histone modifications to their sites of action on the genome. The mammalian Sin3L/Rpd3L complex, comprising more than a dozen different polypeptides, is an ancient HDAC complex found in diverse eukaryotes. The subunits of this complex harbor conserved domains and motifs of unknown structure and function. Here, we show that Sds3, a constitutively-associated subunit critical for the proper functioning of the Sin3L/Rpd3L complex, harbors a type of Tudor domain that we designate the capped Tudor domain. Unlike canonical Tudor domains that bind modified histones, the Sds3 capped Tudor domain binds to nucleic acids that can form higher-order structures such as G-quadruplexes and shares similarities with the knotted Tudor domain of the Esa1 histone acetyltransferase that was previously shown to bind single-stranded RNA. Our findings expand the range of macromolecules capable of recruiting the Sin3L/Rpd3L complex and draw attention to potentially new biological roles for this HDAC complex. American Society for Biochemistry and Molecular Biology 2022-01-01 /pmc/articles/PMC8800102/ /pubmed/34979096 http://dx.doi.org/10.1016/j.jbc.2021.101558 Text en © 2022 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Article
Marcum, Ryan Dale
Hsieh, Joseph
Giljen, Maksim
Justice, Emily
Daffern, Nicolas
Zhang, Yongbo
Radhakrishnan, Ishwar
A capped Tudor domain within a core subunit of the Sin3L/Rpd3L histone deacetylase complex binds to nucleic acid G-quadruplexes
title A capped Tudor domain within a core subunit of the Sin3L/Rpd3L histone deacetylase complex binds to nucleic acid G-quadruplexes
title_full A capped Tudor domain within a core subunit of the Sin3L/Rpd3L histone deacetylase complex binds to nucleic acid G-quadruplexes
title_fullStr A capped Tudor domain within a core subunit of the Sin3L/Rpd3L histone deacetylase complex binds to nucleic acid G-quadruplexes
title_full_unstemmed A capped Tudor domain within a core subunit of the Sin3L/Rpd3L histone deacetylase complex binds to nucleic acid G-quadruplexes
title_short A capped Tudor domain within a core subunit of the Sin3L/Rpd3L histone deacetylase complex binds to nucleic acid G-quadruplexes
title_sort capped tudor domain within a core subunit of the sin3l/rpd3l histone deacetylase complex binds to nucleic acid g-quadruplexes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8800102/
https://www.ncbi.nlm.nih.gov/pubmed/34979096
http://dx.doi.org/10.1016/j.jbc.2021.101558
work_keys_str_mv AT marcumryandale acappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT hsiehjoseph acappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT giljenmaksim acappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT justiceemily acappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT daffernnicolas acappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT zhangyongbo acappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT radhakrishnanishwar acappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT marcumryandale cappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT hsiehjoseph cappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT giljenmaksim cappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT justiceemily cappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT daffernnicolas cappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT zhangyongbo cappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes
AT radhakrishnanishwar cappedtudordomainwithinacoresubunitofthesin3lrpd3lhistonedeacetylasecomplexbindstonucleicacidgquadruplexes

Ejemplares similares