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ADAM12: a genetic modifier of preclinical peripheral arterial disease.


ABSTRACT: In prior studies from multiple groups, outcomes following experimental peripheral arterial disease (PAD) differed considerably across inbred mouse strains. Similarly, in humans with PAD, disease outcomes differ, even when there are similarities in risk factors, disease anatomy, arteriosclerotic burden, and hemodynamic measures. Previously, we identified a locus on mouse chromosome 7, limb salvage-associated quantitative trait locus 1 (LSq-1), which was sufficient to modify outcomes following experimental PAD. We compared expression of genes within LSq-1 in Balb/c mice, which normally show poor outcomes following experimental PAD, with that in C57Bl/6 mice, which normally show favorable outcomes, and found that a disintegrin and metalloproteinase gene 12 (ADAM12) had the most differential expression. Augmentation of ADAM12 expression in vivo improved outcomes following experimental PAD in Balb/c mice, whereas knockdown of ADAM12 made outcomes worse in C57Bl/6 mice. In vitro, ADAM12 expression modulates endothelial cell proliferation, survival, and angiogenesis in ischemia, and this appeared to be dependent on tyrosine kinase with Ig-like and EGF-like domain 2 (Tie2) activation. ADAM12 is sufficient to modify PAD severity in mice, and this likely occurs through regulation of Tie2.

SUBMITTER: Dokun AO 

PROVIDER: S-EPMC4591412 | biostudies-other | 2015 Sep

REPOSITORIES: biostudies-other

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ADAM12: a genetic modifier of preclinical peripheral arterial disease.

Dokun Ayotunde O AO   Chen Lingdan L   Okutsu Mitsuharu M   Farber Charles R CR   Hazarika Surovi S   Jones W Schuyler WS   Craig Damian D   Marchuk Douglas A DA   Lye R John RJ   Shah Svati H SH   Annex Brian H BH  

American journal of physiology. Heart and circulatory physiology 20150710 5


In prior studies from multiple groups, outcomes following experimental peripheral arterial disease (PAD) differed considerably across inbred mouse strains. Similarly, in humans with PAD, disease outcomes differ, even when there are similarities in risk factors, disease anatomy, arteriosclerotic burden, and hemodynamic measures. Previously, we identified a locus on mouse chromosome 7, limb salvage-associated quantitative trait locus 1 (LSq-1), which was sufficient to modify outcomes following exp  ...[more]

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