Redox Stress in Marfan Syndrome: Dissecting the Role of the NADPH Oxidase NOX4 in Aortic Aneurysm

Overview

Journal Free Radic Biol Med

Specialties Biochemistry
Biology
General Medicine

Date 2018 Feb 23

PMID 29471108

Citations 41

Authors

Francesc Jimenez-Altayo

Thayna Meirelles

Eva Crosas-Molist

M Alba Sorolla

Darya Gorbenko Del Blanco

Judit Lopez-Luque

Aleksandra Mas-Stachurska

Ana-Maria Siegert

Fabio Bonorino

Laura Barbera

Carolina Garcia

Enric Condom

Marta Sitges

Fernando Rodriguez-Pascual

Francisco Laurindo

Katrin Schroder

Joaquim Ros

Isabel Fabregat

Gustavo Egea

Affiliations

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Abstract

Marfan syndrome (MFS) is characterized by the formation of ascending aortic aneurysms resulting from altered assembly of extracellular matrix fibrillin-containing microfibrils and dysfunction of TGF-β signaling. Here we identify the molecular targets of redox stress in aortic aneurysms from MFS patients, and investigate the role of NOX4, whose expression is strongly induced by TGF-β, in aneurysm formation and progression in a murine model of MFS. Working models included aortae and cultured vascular smooth muscle cells (VSMC) from MFS patients, and a NOX4-deficient Marfan mouse model (Fbn1-Nox4). Increased tyrosine nitration and reactive oxygen species levels were found in the tunica media of human aortic aneurysms and in cultured VSMC. Proteomic analysis identified nitrated and carbonylated proteins, which included smooth muscle α-actin (αSMA) and annexin A2. NOX4 immunostaining increased in the tunica media of human Marfan aorta and was transcriptionally overexpressed in VSMC. Fbn1-Nox4 mice aortas showed a reduction of fragmented elastic fibers, which was accompanied by an amelioration in the Marfan-associated enlargement of the aortic root. Increase in the contractile phenotype marker calponin in the tunica media of MFS mice aortas was abrogated in Fbn1-Nox4 mice. Endothelial dysfunction evaluated by myography in the Marfan ascending aorta was prevented by the absence of Nox4 or catalase-induced HO decomposition. We conclude that redox stress occurs in MFS, whose targets are actin-based cytoskeleton members and regulators of extracellular matrix homeostasis. Likewise, NOX4 have an impact in the progression of the aortic dilation in MFS and in the structural organization of the aortic tunica media, the VSMC phenotypic modulation, and endothelial function.

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