| Literature DB >> 30559480 |
Florent Laferrière1, Zuzanna Maniecka1, Manuela Pérez-Berlanga1, Marian Hruska-Plochan1, Larissa Gilhespy1, Eva-Maria Hock1, Ulrich Wagner2, Tariq Afroz1, Paul J Boersema3, Gery Barmettler4, Sandrine C Foti5,6, Yasmine T Asi5,6, Adrian M Isaacs6,7, Ashraf Al-Amoudi8, Amanda Lewis8, Henning Stahlberg8, John Ravits9, Francesca De Giorgi10,11,12, François Ichas10,11,12, Erwan Bezard11,12, Paola Picotti4, Tammaryn Lashley5,6, Magdalini Polymenidou13.
Abstract
Accumulation of abnormally phosphorylated TDP-43 (pTDP-43) is the main pathology in affected neurons of people with amyotrophic lateral sclerosis (ALS) and frontotemporal lobar degeneration (FTLD). Morphological diversity and neuroanatomical distribution of pTDP-43 accumulations allowed classification of FTLD cases into at least four subtypes, which are correlated with clinical presentations and genetic causes. To understand the molecular basis of this heterogeneity, we developed SarkoSpin, a new method for biochemical isolation of pathological TDP-43. By combining SarkoSpin with mass spectrometry, we revealed proteins beyond TDP-43 that become abnormally insoluble in a disease subtype-specific manner. We show that pTDP-43 extracted from brain forms stable assemblies of distinct densities and morphologies that are associated with disease subtypes. Importantly, biochemically extracted pTDP-43 assemblies showed differential neurotoxicity and seeding that were correlated with disease duration of FTLD subjects. Our data are consistent with the notion that disease heterogeneity could originate from alternate pathological TDP-43 conformations, which are reminiscent of prion strains.Entities:
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Year: 2018 PMID: 30559480 DOI: 10.1038/s41593-018-0294-y
Source DB: PubMed Journal: Nat Neurosci ISSN: 1097-6256 Impact factor: 24.884