FUS (fused in sarcoma) is a component of the cellular response to topoisomerase I-induced DNA breakage and transcriptional stress

Maria Isabel Martinez-Macias; Duncan Aq Moore; Ryan L Green; Fernando Gomez-Herreros; Marcel Naumann; Andreas Hermann; Philip Van Damme; Majid Hafezparast; Keith W Caldecott

doi:10.26508/lsa.201800222

FUS (fused in sarcoma) is a component of the cellular response to topoisomerase I-induced DNA breakage and transcriptional stress

Life Sci Alliance. 2019 Feb 26;2(2):e201800222. doi: 10.26508/lsa.201800222. Print 2019 Apr.

Authors

Affiliations

¹ Genome Damage and Stability Centre, School of Life Sciences, University of Sussex, Falmer, Brighton, England mm761@sussex.ac.uk.
² Genome Damage and Stability Centre, School of Life Sciences, University of Sussex, Falmer, Brighton, England.
³ Neuroscience, School of Life Sciences, University of Sussex, Falmer, Brighton, England.
⁴ Instituto de Biomedicina de Sevilla, Hospital Virgen del Rocio-Centro Superior de Investigaciones Cientificas-Universidad de Sevilla, Seville, Spain.
⁵ Department of Neurology, Technische Universität Dresden, and German Center for Neurodegenerative Diseases (DZNE), Dresden, Germany.
⁶ Translational Neurodegeneration Section "Albrecht-Kossel", Department of Neurology, University Medical Center Rostock, University of Rostock, Rostock, Germany.
⁷ Center for Transdisciplinary Neurosciences Rostock, University Medical Center Rostock, University of Rostock, Rostock, Germany.
⁸ University of Leuven, Leuven, Belgium.
⁹ Genome Damage and Stability Centre, School of Life Sciences, University of Sussex, Falmer, Brighton, England k.w.caldecott@sussex.ac.uk.

Abstract

FUS (fused in sarcoma) plays a key role in several steps of RNA metabolism, and dominant mutations in this protein are associated with neurodegenerative diseases. Here, we show that FUS is a component of the cellular response to topoisomerase I (TOP1)-induced DNA breakage; relocalising to the nucleolus in response to RNA polymerase II (Pol II) stalling at sites of TOP1-induced DNA breaks. This relocalisation is rapid and dynamic, reversing following the removal of TOP1-induced breaks and coinciding with the recovery of global transcription. Importantly, FUS relocalisation following TOP1-induced DNA breakage is associated with increased FUS binding at sites of RNA polymerase I transcription in ribosomal DNA and reduced FUS binding at sites of RNA Pol II transcription, suggesting that FUS relocates from sites of stalled RNA Pol II either to regulate pre-mRNA processing during transcriptional stress or to modulate ribosomal RNA biogenesis. Importantly, FUS-mutant patient fibroblasts are hypersensitive to TOP1-induced DNA breakage, highlighting the possible relevance of these findings to neurodegeneration.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

A549 Cells
Amyotrophic Lateral Sclerosis / genetics
Amyotrophic Lateral Sclerosis / pathology*
Animals
Binding Sites
Brain / cytology
Brain / embryology
Chromatin / metabolism
DNA Breaks, Double-Stranded*
DNA Repair
DNA Topoisomerases, Type I / metabolism*
Fibroblasts / metabolism
HeLa Cells
Humans
Mice
Mutant Proteins
Mutation / genetics
Neural Stem Cells / metabolism
Neurons / metabolism
RNA Polymerase I / metabolism
RNA Polymerase II / metabolism
RNA-Binding Protein FUS / genetics*
RNA-Binding Protein FUS / metabolism
Transcription, Genetic*

Substances

Chromatin
FUS protein, human
FUS protein, mouse
Mutant Proteins
RNA-Binding Protein FUS
RNA Polymerase II
RNA Polymerase I
DNA Topoisomerases, Type I
TOP1 protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding