SAS-Based Studies of Protein Fibrillation

Carlotta Marasini, Bente Vestergaard

Research output: Chapter in Book/Report/Conference proceedingBook chapterResearchpeer-review

1 Citation (Scopus)

Abstract

Protein fibrillation is associated with a number of fatal amyloid diseases (e.g. Alzheimer's and Parkinson's diseases). From a structural point of view, the aggregation process starts from an ensemble of native states that convert into transiently formed oligomers, higher order assemblies and protofibrils and, finally, fibrils. The different species exist in equilibrium in solution leading to a high degree of sample heterogeneity. It is impossible to physically isolate any single species for structural analysis: separation will alter the equilibrium and potentially cause structural changes.Small angle scattering is an optimal method for structural studies of the fibrillation process in order to further the knowledge of the associated diseases. The recorded scattering data include the scattering contribution of all the species in solution and must be decomposed to enable structural modeling of the individual components involved during the fibrillation, notably without physical separation of the species. In this chapter we explain how to optimize a small angle scattering analysis of the fibrillation process and the basic principles behind analysis of the data. We include several practical tips and highlight existing reports, exemplifying the wealth of information that can be derived from the method.

Original languageEnglish
Title of host publicationBiological Small Angle Scattering: Techniques, Strategies and Tips
Number of pages17
Volume1009
PublisherSpringer Science+Business Media
Publication date2017
Pages149-165
DOIs
Publication statusPublished - 2017
SeriesAdvances in Experimental Medicine and Biology
ISSN0065-2598

Keywords

  • Journal Article

Cite this