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Lipids uniquely alter secondary structure and toxicity of lysozyme aggregates

Mikhail Matveyenka, Kiryl Zhaliazka, Stanislav Rizevsky, Dmitry Kurouski

2022The FASEB Journal34 citationsDOIOpen Access PDF

Abstract

Abrupt aggregation of misfolded proteins is a hallmark of the large group of amyloid pathologies that include diabetes type 2, Alzheimer and Parkinson's diseases. Protein aggregation yields oligomers and fibrils, β-sheet-rich structures that exert cell toxicity. Microscopic examination of amyloid deposits reveals the presence of lipids membranes, which suggests that lipids can be involved in the process of pathogenic protein assembly. In this study, we show that lipids can uniquely alter the aggregation rates of lysozyme, a protein that is associated with systemic amyloidosis. Specifically, cardiolipin (CL), ceramide (CER), and sphingomyelin (SM) accelerate, phosphatidylcholine (PC) strongly inhibits, whereas phosphatidylserine (PS) has no effect on the rate of protein aggregation. Furthermore, lipids uniquely alter the secondary structure of lysozyme aggregates. Furthermore, we found that lysozyme aggregates grown in the presence of CL, CER, SM, PS, and CL:PC mixtures exert significantly lower production of reactive oxygen species and mitochondrial dysfunction compared to lysozyme:PC aggregates and lysozyme fibrils grown in the lipid-free environment. These findings suggest that a change in the lipid composition of cell membranes, which is taken place upon neurodegeneration, may trigger the formation of toxic protein species that otherwise would not be formed.

Topics & Concepts

LysozymeToxicityChemistryBiophysicsEnvironmental chemistryBiochemistryBiologyOrganic chemistryLipid Membrane Structure and BehaviorProtein Structure and DynamicsProtein Interaction Studies and Fluorescence Analysis
Lipids uniquely alter secondary structure and toxicity of lysozyme aggregates | Litcius