Litcius/Paper detail

Zinc ions prevent α-synuclein aggregation by enhancing chaperone function of human serum albumin

Samah Al-Harthi, Vladlena Kharchenko, Papita Mandal, Spyridon Gourdoupis, Łukasz Jaremko

2022International Journal of Biological Macromolecules25 citationsDOIOpen Access PDF

Abstract

Metal ions present in cellular microenvironment have been implicated as drivers of aggregation of amyloid forming proteins. Zinc (Zn2+) ions have been reported to directly interact with α-synuclein (AS), a causative agent of Parkinson's disease and other neurodegenerative diseases, and promote its aggregation. AS is a small intrinsically disordered protein (IDP) i.e., understanding molecular factors that drive its misfolding and aggregation has been challenging since methods used routinely to study protein structure are not effective for IDPs. Here, we report the atomic details of Zn2+ binding to AS at physiologically relevant conditions using proton-less NMR techniques that can be applied to highly dynamic systems like IDPs. We also examined how human serum albumin (HSA), the most abundant protein in human blood, binds to AS and whether Zn2+ and/or ionic strength affect this. We conclude that Zn2+ enhances the anti-aggregation chaperoning role of HSA that relies on protecting the hydrophobic N-terminal and NAC regions of AS, rather than polar negatively charged C-terminus. This suggested a previously undocumented role of Zn2+ in HSA function and AS aggregation.

Topics & Concepts

Human serum albuminChemistryBiophysicsProtein aggregationChaperone (clinical)Intrinsically disordered proteinsPlasma protein bindingIonic strengthSynucleinFunction (biology)ZincMetal ions in aqueous solutionAlpha-synucleinBiochemistryIonCell biologyBiologyParkinson's diseaseAqueous solutionMedicinePhysical chemistryPathologyDiseaseOrganic chemistryParkinson's Disease Mechanisms and TreatmentsAlzheimer's disease research and treatmentsTrace Elements in Health