| Literature DB >> 34338090 |
Jonathan Schönfelder1, Peter Benedikt Pfeiffer1, Tejaswini Pradhan2, Johan Bijzet3, Bouke P C Hazenberg3, Stefan O Schönland4, Ute Hegenbart4, Bernd Reif2, Christian Haupt1, Marcus Fändrich1.
Abstract
Several studies recently showed that ex vivo fibrils from patient or animal tissue were structurally different from in vitro formed fibrils from the same polypeptide chain. Analysis of serum amyloid A (SAA) and Aβ-derived amyloid fibrils additionally revealed that ex vivo fibrils were more protease stable than in vitro fibrils. These observations gave rise to the proteolytic selection hypothesis that suggested that disease-associated amyloid fibrils were selected inside the body by their ability to resist endogenous clearance mechanisms. We here show, for more than twenty different fibril samples, that ex vivo fibrils are more protease stable than in vitro fibrils. These data support the idea of a proteolytic selection of pathogenic amyloid fibril morphologies and help to explain why only few amino acid sequences lead to amyloid diseases, although many, if not all, polypeptide chains can form amyloid fibrils in vitro.Entities:
Keywords: Amyloid structure; prion; protein misfolding; proteolytic stability; immunoglobulin light chain; transthyretin; serum amyloid A
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Year: 2021 PMID: 34338090 DOI: 10.1080/13506129.2021.1960501
Source DB: PubMed Journal: Amyloid ISSN: 1350-6129 Impact factor: 7.141