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10.1038/ncomms8831

http://scihub22266oqcxt.onion/10.1038/ncomms8831
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C4525161!4525161!26215704
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suck abstract from ncbi


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pmid26215704      Nat+Commun 2015 ; 6 (ä): ä
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  • Infrared nanospectroscopy characterization of oligomeric and fibrillar aggregates during amyloid formation #MMPMID26215704
  • Ruggeri FS; Longo G; Faggiano S; Lipiec E; Pastore A; Dietler G
  • Nat Commun 2015[]; 6 (ä): ä PMID26215704show ga
  • Amyloids are insoluble protein fibrillar aggregates. The importance of characterizing their aggregation has steadily increased because of their link to human diseases and material science applications. In particular, misfolding and aggregation of the Josephin domain of ataxin-3 is implicated in spinocerebellar ataxia-3. Infrared nanospectroscopy, simultaneously exploiting atomic force microscopy and infrared spectroscopy, can characterize at the nanoscale the conformational rearrangements of proteins during their aggregation. Here we demonstrate that we can individually characterize the oligomeric and fibrillar species formed along the amyloid aggregation. We describe their secondary structure, monitoring at the nanoscale an ?-to-? transition, and couple these studies with an independent measurement of the evolution of their intrinsic stiffness. These results suggest that the aggregation of Josephin proceeds from the monomer state to the formation of spheroidal intermediates with a native structure. Only successively, these intermediates evolve into misfolded aggregates and into the final fibrils.
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