Pathological apoptosis by xanthurenic acid, a tryptophan metabolite: activation of cell caspases but not cytoskeleton breakdown

A family of aspartate-specific cysteinyl proteases, named caspases, mediates programmed cell death, apoptosis. In this function, caspases are important for physiological processes such as development and maintenance of organ homeostasis. Caspases are, however, also engaged in aging and disease devel...

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Published inBMC physiology Vol. 1; no. 1; p. 7
Main Authors Malina, H Z, Richter, C, Mehl, M, Hess, O M
Format Journal Article
LanguageEnglish
Published England BioMed Central Ltd 04.07.2001
BioMed Central
Subjects
Aging
Apoptosis
Caspase 3
Caspases - metabolism
Cytoskeleton - drug effects
Cytoskeleton - ultrastructure
Enzyme Activation
Health aspects
Humans
Medical examination
Middle Aged
Mitochondria - drug effects
Muscle, Smooth, Vascular - drug effects
Muscle, Smooth, Vascular - enzymology
Muscle, Smooth, Vascular - ultrastructure
Smooth muscle
Tryptophan - metabolism
Xanthurenates - metabolism
Xanthurenates - toxicity
Switzerland
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Summary:A family of aspartate-specific cysteinyl proteases, named caspases, mediates programmed cell death, apoptosis. In this function, caspases are important for physiological processes such as development and maintenance of organ homeostasis. Caspases are, however, also engaged in aging and disease development. The factors inducing age-related caspase activation are not known. Xanthurenic acid, a product of tryptophan degradation, is present in blood and urine, and accumulates in organs with aging. Here, we report triggering of apoptotic key events by xanthurenic acid in vascular smooth muscle and retinal pigment epithelium cells. Upon exposure of these cells to xanthurenic acid a degradation of ICAD/DFF45, poly(ADP-ribose) polymerase, and gelsolin was observed, giving a pattern of protein cleavage characteristic for caspase-3 activity. Active caspase-3, -8 and caspase-9 were detected by Western blot analysis and immunofluorescence. In the presence of xanthurenic acid the amino-terminal fragment of gelsolin bound to the cytoskeleton, but did not lead to the usually observed cytoskeleton breakdown. Xanthurenic acid also caused mitochondrial migration, cytochrome C release, and destruction of mitochondria and nuclei. These results indicate that xanthurenic acid is a previously not recognized endogenous cell death factor. Its accumulation in cells may lead to accelerated caspase activation related to aging and disease development.
ISSN:1472-6793
1472-6793
DOI:10.1186/1472-6793-1-7