Oxidative stress and mitochondrial dysfunction in Kindler syndrome

authors

ZAPATERO SOLANA, ELISABET
GARCIA-GIMENEZ, JOSE LUIS
GUERRERO ASPIZUA, SARA
GARCIA DIEZ, MARTA
TOLL, AGUSTI
BASELGA TORRES, EULALIA
DURAN-MORENO, MARIA
MARKOVIC, JELENA
GARCIA-VERDUGO, JOSE MANUEL
CONTI, CLAUDIO JORGE
HAS, CRISTINA
LARCHER LAGUZZI, FERNANDO
PALLARDO, FEDERICO V.
RIO NECHAEVSKY, MARCELA ANDREA DEL

published in

Orphanet Journal of Rare Diseases Journal

publication date

December 2014

start page

1

end page

10

volume

9:211

Digital Object Identifier (DOI)

https://doi.org/10.1186/s13023-014-0211-8

Electronic International Standard Serial Number (EISSN)

1750-1172

abstract

Background: Kindler Syndrome (KS) is an autosomal recessive skin disorder characterized by skin blistering, photosensitivity, premature aging, and propensity to skin cancer. In spite of the knowledge underlying cause of this disease involving mutations of FERMT1 (fermitin family member 1), and efforts to characterize genotype-phenotype correlations, the clinical variability of this genodermatosis is still poorly understood. In addition, several pathognomonic features of KS, not related to skin fragility such as aging, inflammation and cancer predisposition have been strongly associated with oxidative stress. Alterations of the cellular redox status have not been previously studied in KS. Here we explored the role of oxidative stress in the pathogenesis of this rare cutaneous disease.Methods: Patient-derived keratinocytes and their respective controls were cultured and classified according to their different mutations by PCR and western blot, the oxidative stress biomarkers were analyzed by spectrophotometry and qPCR and additionally redox biosensors experiments were also performed. The mitochondrial structure and functionality were analyzed by confocal microscopy and electron microscopy. Results: Patient-derived keratinocytes showed altered levels of several oxidative stress biomarkers including MDA (malondialdehyde), GSSG/GSH ratio (oxidized and reduced glutathione) and GCL (gamma-glutamyl cysteine ligase) subunits. Electron microscopy analysis of both, KS skin biopsies and keratinocytes showed marked morphological mitochondrial abnormalities. Consistently, confocal microscopy studies of mitochondrial fluorescent probes confirmed the mitochondrial derangement. Imbalance of oxidative stress biomarkers together with abnormalities in the mitochondrial network and function are consistent with a pro-oxidant state.Conclusions: This is the first study to describe mitochondrial dysfunction and oxidative stress involvement in KS.

Oxidative stress and mitochondrial dysfunction in Kindler syndrome Articles

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