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Repeat length increases disease penetrance and severity in <i>C9orf72</i> ALS/FTD BAC transgenic mice

Amrutha Pattamatta, Lien Nguyen, Hailey Olafson, Marina M. Scotti, Lauren A. Laboissonniere, Jared Richardson, J. Andrew Berglund, Tao Zu, Eric T. Wang, Laura P.W. Ranum

2020Human Molecular Genetics18 citationsDOIOpen Access PDF

Abstract

C9orf72 ALS/FTD patients show remarkable clinical heterogeneity, but the complex biology of the repeat expansion mutation has limited our understanding of the disease. BAC transgenic mice were used to better understand the molecular mechanisms and repeat length effects of C9orf72 ALS/FTD. Genetic analyses of these mice demonstrate that the BAC transgene and not integration site effects cause ALS/FTD phenotypes. Transcriptomic changes in cell proliferation, inflammation and neuronal pathways are found late in disease and alternative splicing changes provide early molecular markers that worsen with disease progression. Isogenic sublines of mice with 800, 500 or 50 G4C2 repeats generated from the single-copy C9-500 line show longer repeats result in earlier onset, increased disease penetrance and increased levels of RNA foci and dipeptide RAN protein aggregates. These data demonstrate G4C2 repeat length is an important driver of disease and identify alternative splicing changes as early biomarkers of C9orf72 ALS/FTD.

Topics & Concepts

BiologyC9orf72PenetranceTransgeneGeneticsGenetically modified mouseDiseaseTrinucleotide repeat expansionMolecular biologyGenePhenotypeAlleleInternal medicineMedicineAmyotrophic Lateral Sclerosis ResearchPrion Diseases and Protein MisfoldingBiochemical Acid Research Studies