Šušnjar, Urša; Škrabar, Neva; Brown, Anna-Leigh; Abbassi, Yasmine; Phatnani, Hemali; NYGC ALS Consortium, .; Cortese, Andrea; ... Buratti, Emanuele; + view all Šušnjar, Urša; Škrabar, Neva; Brown, Anna-Leigh; Abbassi, Yasmine; Phatnani, Hemali; NYGC ALS Consortium, .; Cortese, Andrea; Cereda, Cristina; Bugiardini, Enrico; Cardani, Rosanna; Meola, Giovanni; Ripolone, Michela; Moggio, Maurizio; Romano, Maurizio; Secrier, Maria; Fratta, Pietro; Buratti, Emanuele; - view fewer (2022) Cell environment shapes TDP-43 function with implications in neuronal and muscle disease. Communications Biology , 5 , Article 314. 10.1038/s42003-022-03253-8.

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Abstract

TDP-43 (TAR DNA-binding protein 43) aggregation and redistribution are recognised as a hallmark of amyotrophic lateral sclerosis and frontotemporal dementia. As TDP-43 inclusions have recently been described in the muscle of inclusion body myositis patients, this highlights the need to understand the role of TDP-43 beyond the central nervous system. Using RNA-seq, we directly compare TDP-43-mediated RNA processing in muscle (C2C12) and neuronal (NSC34) mouse cells. TDP-43 displays a cell-type-characteristic behaviour targeting unique transcripts in each cell-type, which is due to characteristic expression of RNA-binding proteins, that influence TDP-43's performance and define cell-type specific splicing. Among splicing events commonly dysregulated in both cell lines, we identify some that are TDP-43-dependent also in human cells. Inclusion levels of these alternative exons are altered in tissues of patients suffering from FTLD and IBM. We therefore propose that TDP-43 dysfunction contributes to disease development either in a common or a tissue-specific manner.

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