Published April 16, 2021 | Version v1
Publication Metadata-only

Autophagic receptor p62 protects against glycation-derived toxicity and enhances viability

Aragonès, Gemma
Dasuri, Kalavathi
Olukorede, Opeoluwa
Francisco, Sarah G.
Renneburg, Carol
Kumsta, Caroline
Daza Navarro, María Paula
Ruano Caballero, Diego
Domínguez Martín, Helena
Taylor, Allen
Others:
Universidad de Sevilla. Departamento de Bioquímica y Biología Molecular
Universidad de Sevilla. Departamento de Biología Celular

Description

Diabetes and metabolic syndrome are associated with the typical American high glycemia diet and result in accumulation of high levels of advanced glycation end products (AGEs), particularly upon aging. AGEs form when sugars or their metabolites react with proteins. Associated with a myriad of age-related diseases, AGEs accumulate in many tissues and are cytotoxic. To date, efforts to limit glycation pharmacologically have failed in human trials. Thus, it is crucial to identify systems that remove AGEs, but such research is scanty. Here, we determined if and how AGEs might be cleared by autophagy. Our in vivo mouse and C. elegans models, in which we altered proteolysis or glycative burden, as well as experiments in five types of cells, revealed more than six criteria indicating that p62-dependent autophagy is a conserved pathway that plays a critical role in the removal of AGEs. Activation of autophagic removal of AGEs requires p62, and blocking this pathway results in accumulation of AGEs and compromised viability. Deficiency of p62 accelerates accumulation of AGEs in soluble and insoluble fractions. p62 itself is subject to glycative inactivation and accumulates as high mass species. Accumulation of p62 in retinal pigment epithelium is reversed by switching to a lower glycemia diet. Since diminution of glycative damage is associated with reduced risk for age-related diseases, including age-related macular degeneration, cardiovascular disease, diabetes, Alzheimer's, and Parkinson's, discovery of methods to limit AGEs or enhance p62-dependent autophagy offers novel potential therapeutic targets to treat AGEs-related pathologies.

Abstract

National Institutes of Health R01AG028664, R21AG058038, R01EY021212, R01EY026979, R01EY028559

Abstract

U.S. Department of Agriculture 8050-51000-089-01S

Abstract

Human Nutrition Research Center on Aging 2016–08885

Abstract

Ministerio de Economía y Competitividad SAF 2016 78666‐R

Additional details

Identifiers Origin repository
Created:
March 27, 2023
Modified:
November 29, 2023