Tuning the rate of aggregation of hIAPP into amyloid using small-molecule modulators of assembly

Author:

Xu YongORCID,Maya-Martinez Roberto,Guthertz Nicolas,Heath George R.ORCID,Manfield Iain W.ORCID,Breeze Alexander L.ORCID,Sobott FrankORCID,Foster Richard,Radford Sheena E.ORCID

Abstract

AbstractHuman islet amyloid polypeptide (hIAPP) self-assembles into amyloid fibrils which deposit in pancreatic islets of type 2 diabetes (T2D) patients. Here, we applied chemical kinetics to study the mechanism of amyloid assembly of wild-type hIAPP and its more amyloidogenic natural variant S20G. We show that the aggregation of both peptides involves primary nucleation, secondary nucleation and elongation. We also report the discovery of two structurally distinct small-molecule modulators of hIAPP assembly, one delaying the aggregation of wt hIAPP, but not S20G; while the other enhances the rate of aggregation of both variants at substoichiometric concentrations. Investigation into the inhibition mechanism(s) using chemical kinetics, native mass spectrometry, fluorescence titration, SPR and NMR revealed that the inhibitor retards primary nucleation, secondary nucleation and elongation, by binding peptide monomers. By contrast, the accelerator predominantly interacts with species formed in the lag phase. These compounds represent useful chemical tools to study hIAPP aggregation and may serve as promising starting-points for the development of therapeutics for T2D.

Funder

Royal Society

RCUK | Biotechnology and Biological Sciences Research Council

RCUK | Engineering and Physical Sciences Research Council

Wellcome Trust

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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