Nuclear inclusions of pathogenic ataxin-1 induce oxidative stress and perturb the protein synthesis machinery

6533b824fe1ef96bd12801cf

RESEARCH PRODUCT

Nuclear inclusions of pathogenic ataxin-1 induce oxidative stress and perturb the protein synthesis machinery

Fotis Psomopoulos Zoltán Ivics Boris Tichy Maria Lefaki Zsuzsanna Izsvák Maria Tsagiopoulou Gregorio Alanis-lobato ŠáRka Pospíšilová Jan Pribyl Niki Chondrogianni Georgia Kastrinaki Tamás Raskó Spyros Petrakis Petr Skládal Kamil Mikulášek Alessandro Prigione Manvendra K. Singh Stamatia Laidou Miguel A. Andrade-navarro Jan Oppelt Annika Zink

subject

0301 basic medicine SCA1 Spinocerebellar ataxia type-1 Intranuclear Inclusion Bodies Clinical Biochemistry MSC mesenchymal stem cell Protein aggregation Biochemistry 0302 clinical medicine Mutant protein Protein biosynthesis DE differentially expressed genes Nuclear protein lcsh:QH301-705.5 FTIR Fourier-transform infrared spectroscopy Ataxin-1 lcsh:R5-920 biology Chemistry Nuclear Proteins polyQ polyglutamine Ribosome Cell biology SB Sleeping Beauty Ribosome ; Polyglutamine ; Ataxin-1 ; Oxidative stress ; Transposon ; Sleeping beauty transposon ; Protein network Spinocerebellar ataxia Protein folding Cellular model Function and Dysfunction of the Nervous System lcsh:Medicine (General)Research Paper iPSC induced pluripotent stem cell Ataxin 1 Nerve Tissue Proteins PPI protein-protein interaction 03 medical and health sciences ROS reactive oxygen species Protein network Sleeping beauty transposon GSEA Gene Set Enrichment Analysis medicine Humans NPC neural progenitor cell Organic Chemistry medicine.disease AFM atomic force microscopy Oxidative Stress 030104 developmental biology lcsh:Biology (General)IIBs intranuclear inclusion bodies MS mass spectrometry Cardiovascular and Metabolic Diseases biology.protein Polyglutamine 030217 neurology & neurosurgery

description

Spinocerebellar ataxia type-1 (SCA1) is caused by an abnormally expanded polyglutamine (polyQ) tract in ataxin-1. These expansions are responsible for protein misfolding and self-assembly into intranuclear inclusion bodies (IIBs) that are somehow linked to neuronal death. However, owing to lack of a suitable cellular model, the downstream consequences of IIB formation are yet to be resolved. Here, we describe a nuclear protein aggregation model of pathogenic human ataxin-1 and characterize IIB effects. Using an inducible Sleeping Beauty transposon system, we overexpressed the ATXN1(Q82) gene in human mesenchymal stem cells that are resistant to the early cytotoxic effects caused by the expression of the mutant protein. We characterized the structure and the protein composition of insoluble polyQ IIBs which gradually occupy the nuclei and are responsible for the generation of reactive oxygen species. In response to their formation, our transcriptome analysis reveals a cerebellum-specific perturbed protein interaction network, primarily affecting protein synthesis. We propose that insoluble polyQ IIBs cause oxidative and nucleolar stress and affect the assembly of the ribosome by capturing or down-regulating essential components. The inducible cell system can be utilized to decipher the cellular consequences of polyQ protein aggregation. Our strategy provides a broadly applicable methodology for studying polyQ diseases.

year	journal	country	edition	language
2020-05-01

10.1016/j.redox.2020.101458 https://www.sciencedirect.com/science/article/pii/S2213231719312947?via=ihub#appsec1