Suppression of UVA-mediated Release of Labile Iron by Epicatechin--a Link to Lysosomal Protection

Overview

Journal Free Radic Biol Med

Specialties Biochemistry
Biology
General Medicine

Date 2006 Oct 4

PMID 17015166

Citations 12

Authors

Sharmila Basu-Modak

Dalia Ali

Matt Gordon

Tobias Polte

Anthie Yiakouvaki

Charareh Pourzand

Catherine Rice-Evans

Rex M Tyrrell

Affiliations

Soon will be listed here.

Abstract

UVA (320-380 nm) radiation generates an oxidative stress in cells and leads to an immediate release of potentially damaging labile iron pools in human skin cells. Treatment of cultured skin fibroblasts for several hours with physiologically relevant concentrations of either epicatechin (EC), a flavonoid plant constituent present in foods, or methylated epicatechin (3'-O-methyl epicatechin, MeOEC), its major human metabolite, prevents this iron release. The similarity of the effectiveness of EC and MeOEC argues against chelation as the mechanism of iron removal. Evidence based on measurements of lysosomal integrity strongly supports the hypothesis that the catechins protect against lysosomal destruction by UVA. Such damage would normally lead to protease release, which has been previously shown to cause ferritin degradation and release of labile iron.

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