About: Deletion of the α8 Integrin Gene Does Not Protect Mice From Myocardial Fibrosis in DOCA Hypertension

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Attributs	Valeurs
type	work Article
Is Part Of	http://hub.abes.fr/oup/periodical/ajh/2009/volume_22/issue_1/w
Subject	Articles ORIGINAL CONTRIBUTIONS
Title	Deletion of the α8 Integrin Gene Does Not Protect Mice From Myocardial Fibrosis in DOCA Hypertension
has manifestation of work	http://hub.abes.fr/oup/periodical/ajh/2009/volume_22/issue_1/101038ajh2008309/m/web http://hub.abes.fr/oup/periodical/ajh/2009/volume_22/issue_1/101038ajh2008309/m/print
related by	http://hub.abes.fr/oup/periodical/ajh/2009/volume_22/issue_1/101038ajh2008309/authorship/4 http://hub.abes.fr/oup/periodical/ajh/2009/volume_22/issue_1/101038ajh2008309/authorship/3 http://hub.abes.fr/oup/periodical/ajh/2009/volume_22/issue_1/101038ajh2008309/authorship/1 http://hub.abes.fr/oup/periodical/ajh/2009/volume_22/issue_1/101038ajh2008309/authorship/2
Author	Cordasic Nada Hilgers Karl F. Rascher Wolfgang Hartner Andrea
Abstract	Background. In the heart, the α8 integrin chain is expressed in fibroblasts and vascular smooth-muscle cells but its functional role in the myocardium is unknown. Integrins can contribute to tissue fibrosis in several organs. We tested the hypothesis that α8 integrin-mediated cell-matrix interactions add to cardiac fibrotic alterations during hypertension. Methods. Desoxycorticosterone-acetate (DOCA)-salt hypertension was induced in mice homozygous for a deletion of the α8 integrin chain and wild-type mice. Histological and immunohistochemical evaluations were performed in heart tissue. Results. Blood pressure was slightly higher in DOCA-treated α8 integrin-deficient mice compared to DOCA-treated wild types. Expression of α8 integrin and its ligands fibronectin and osteopontin was increased in the hearts of DOCA-treated wild types compared to salt-loaded controls. However, relative left ventricular weights did not differ between DOCA-treated wild types and α8 integrin-deficient mice. Moreover, expansion of collagen I immunoreactivity and cell proliferation was similar in both groups. The number of osteopontin-positive cells was not different in DOCA-treated α8 integrin-deficient and DOCA-treated wild-type mice. Despite of a comparable degree of fibrosis in both groups, α-smooth-muscle actin and discoidin domain receptor 2 (DDR2)-positive myofibroblasts were only detected in wild-type DOCA-treated mice, not in DOCA-treated α8 integrin-deficient mice. Conclusions. The results show that lack of α8 integrin does not reduce fibrotic changes in the hearts of DOCA-salt hypertensive mice. Our findings do not argue for a profibrotic effect of an increased α8 integrin expression in the myocardium in hypertension. . American Journal of Hypertension (2009). doi:10.1038/ajh.2008.309
article type	research-article
is part of this journal	American Journal of Hypertension

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