ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cells

ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cells

Abstract Genes encoding replication-dependent histones lack introns, and the mRNAs produced are a unique class of RNA polymerase II transcripts in eukaryotic cells that do not end in a polyadenylated tail. Mature mRNAs are thus formed by a single endonucleolytic cleavage that releases the pre-mRNA f...

Full description

Bibliographic Details
Main Authors: Ankur Gadgil, Agnieszka Walczak, Agata Stępień, Jonas Mechtersheimer, Agnes Lumi Nishimura, Christopher E. Shaw, Marc-David Ruepp, Katarzyna Dorota Raczyńska
Format: Article
Language:English
Published: Nature Publishing Group 2021-06-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-021-91453-3
id doaj-cc016ad4171f42469bc5c1df58514821
record_format Article
spelling doaj-cc016ad4171f42469bc5c1df585148212021-06-06T11:39:55ZengNature Publishing GroupScientific Reports2045-23222021-06-011111910.1038/s41598-021-91453-3ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cellsAnkur Gadgil0Agnieszka Walczak1Agata Stępień2Jonas Mechtersheimer3Agnes Lumi Nishimura4Christopher E. Shaw5Marc-David Ruepp6Katarzyna Dorota Raczyńska7Department of Gene Expression, Institute of Molecular Biology and Biotechnology, Faculty of Biology, Adam Mickiewicz UniversityDepartment of Gene Expression, Institute of Molecular Biology and Biotechnology, Faculty of Biology, Adam Mickiewicz UniversityDepartment of Gene Expression, Institute of Molecular Biology and Biotechnology, Faculty of Biology, Adam Mickiewicz UniversityUK Dementia Research Institute Centre at King’s College London, Institute of Psychiatry, Psychology and Neuroscience, King’s College LondonUK Dementia Research Institute Centre at King’s College London, Institute of Psychiatry, Psychology and Neuroscience, King’s College LondonUK Dementia Research Institute Centre at King’s College London, Institute of Psychiatry, Psychology and Neuroscience, King’s College LondonUK Dementia Research Institute Centre at King’s College London, Institute of Psychiatry, Psychology and Neuroscience, King’s College LondonDepartment of Gene Expression, Institute of Molecular Biology and Biotechnology, Faculty of Biology, Adam Mickiewicz UniversityAbstract Genes encoding replication-dependent histones lack introns, and the mRNAs produced are a unique class of RNA polymerase II transcripts in eukaryotic cells that do not end in a polyadenylated tail. Mature mRNAs are thus formed by a single endonucleolytic cleavage that releases the pre-mRNA from the DNA and is the only processing event necessary. U7 snRNP is one of the key factors that determines the cleavage site within the 3ʹUTR of replication-dependent histone pre-mRNAs. We have previously showed that the FUS protein interacts with U7 snRNA/snRNP and regulates the expression of histone genes by stimulating transcription and 3ʹ end maturation. Mutations in the FUS gene first identified in patients with amyotrophic lateral sclerosis (ALS) lead to the accumulation of the FUS protein in cytoplasmic inclusions. Here, we report that mutations in FUS lead to disruption of the transcriptional activity of FUS and mislocalization of U7 snRNA/snRNP in cytoplasmic aggregates in cellular models and primary neurons. As a consequence, decreased transcriptional efficiency and aberrant 3ʹ end processing of histone pre-mRNAs were observed. This study highlights for the first time the deregulation of replication-dependent histone gene expression and its involvement in ALS.https://doi.org/10.1038/s41598-021-91453-3
collection DOAJ
language English
format Article
sources DOAJ
author Ankur Gadgil
Agnieszka Walczak
Agata Stępień
Jonas Mechtersheimer
Agnes Lumi Nishimura
Christopher E. Shaw
Marc-David Ruepp
Katarzyna Dorota Raczyńska
spellingShingle Ankur Gadgil
Agnieszka Walczak
Agata Stępień
Jonas Mechtersheimer
Agnes Lumi Nishimura
Christopher E. Shaw
Marc-David Ruepp
Katarzyna Dorota Raczyńska
ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cells
Scientific Reports
author_facet Ankur Gadgil
Agnieszka Walczak
Agata Stępień
Jonas Mechtersheimer
Agnes Lumi Nishimura
Christopher E. Shaw
Marc-David Ruepp
Katarzyna Dorota Raczyńska
author_sort Ankur Gadgil
title ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cells
title_short ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cells
title_full ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cells
title_fullStr ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cells
title_full_unstemmed ALS-linked FUS mutants affect the localization of U7 snRNP and replication-dependent histone gene expression in human cells
title_sort als-linked fus mutants affect the localization of u7 snrnp and replication-dependent histone gene expression in human cells
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-06-01
description Abstract Genes encoding replication-dependent histones lack introns, and the mRNAs produced are a unique class of RNA polymerase II transcripts in eukaryotic cells that do not end in a polyadenylated tail. Mature mRNAs are thus formed by a single endonucleolytic cleavage that releases the pre-mRNA from the DNA and is the only processing event necessary. U7 snRNP is one of the key factors that determines the cleavage site within the 3ʹUTR of replication-dependent histone pre-mRNAs. We have previously showed that the FUS protein interacts with U7 snRNA/snRNP and regulates the expression of histone genes by stimulating transcription and 3ʹ end maturation. Mutations in the FUS gene first identified in patients with amyotrophic lateral sclerosis (ALS) lead to the accumulation of the FUS protein in cytoplasmic inclusions. Here, we report that mutations in FUS lead to disruption of the transcriptional activity of FUS and mislocalization of U7 snRNA/snRNP in cytoplasmic aggregates in cellular models and primary neurons. As a consequence, decreased transcriptional efficiency and aberrant 3ʹ end processing of histone pre-mRNAs were observed. This study highlights for the first time the deregulation of replication-dependent histone gene expression and its involvement in ALS.
url https://doi.org/10.1038/s41598-021-91453-3
work_keys_str_mv AT ankurgadgil alslinkedfusmutantsaffectthelocalizationofu7snrnpandreplicationdependenthistonegeneexpressioninhumancells
AT agnieszkawalczak alslinkedfusmutantsaffectthelocalizationofu7snrnpandreplicationdependenthistonegeneexpressioninhumancells
AT agatastepien alslinkedfusmutantsaffectthelocalizationofu7snrnpandreplicationdependenthistonegeneexpressioninhumancells
AT jonasmechtersheimer alslinkedfusmutantsaffectthelocalizationofu7snrnpandreplicationdependenthistonegeneexpressioninhumancells
AT agnesluminishimura alslinkedfusmutantsaffectthelocalizationofu7snrnpandreplicationdependenthistonegeneexpressioninhumancells
AT christophereshaw alslinkedfusmutantsaffectthelocalizationofu7snrnpandreplicationdependenthistonegeneexpressioninhumancells
AT marcdavidruepp alslinkedfusmutantsaffectthelocalizationofu7snrnpandreplicationdependenthistonegeneexpressioninhumancells
AT katarzynadorotaraczynska alslinkedfusmutantsaffectthelocalizationofu7snrnpandreplicationdependenthistonegeneexpressioninhumancells
_version_ 1721393772232704000

Similar Items