Chronic Treatment with a Broad-Spectrum Metalloproteinase Inhibitor, Doxycycline, Prevents the Development of Spontaneous Aortic Lesions in a Mouse Model of Vascular Ehlers-Danlos Syndrome

Tae, Hyun‐Jin; Marshall, Shannon; Zhang, Jing; Wang, Mingyi; Briest, Wilfried; Talan, Mark I.

doi:10.1124/jpet.112.197020

Cited by 26 publications

(15 citation statements)

References 38 publications

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“…Interestingly, aging increases MMP-2-cleaved elastin and activated TGF-β1/TGF-β receptor type II signaling, contributes to increased production of collagen I, II, III, and the biologic glue, fibronectin, and leads to elastin fragmentation and fibrosis [ 146 , 147 ]. In addition to increases in MMP-2 activity, activation of the intracellular calcium-dependent proteinase, calpain-1, is also involved in TGF-β1 activation and increased collagen production in old VSMCs [ 146 ] .…”

Section: Proinflammatory Cellular Phenotypic Changes During Cardiovasmentioning

confidence: 99%

Age-associated pro-inflammatory remodeling and functional phenotype in the heart and large arteries

Wang

Shah

2015

Journal of Molecular and Cellular Cardiology

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The aging population is increasing dramatically. Aging–associated stress simultaneously drives proinflammatory remodeling, involving angiotensin II and other factors, in both the heart and large arteries. The structural remodeling and functional changes that occur with aging include cardiac and vascular wall stiffening, systolic hypertension and suboptimal ventricular-arterial coupling, features that are often clinically silent and thus termed a silent syndrome. These age-related effects are the result of responses initiated by cardiovascular proinflammatory cells. Local proinflammatory signals are coupled between the heart and arteries due to common mechanical and humoral messengers within a closed circulating system. Thus, targeting proinflammatory signaling molecules would be a promising approach to improve age-associated suboptimal ventricular-arterial coupling, a major predisposing factor for the pathogenesis of clinical cardiovascular events such as heart failure.

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Section: Proinflammatory Cellular Phenotypic Changes During Cardiovasmentioning

confidence: 99%

Age-associated pro-inflammatory remodeling and functional phenotype in the heart and large arteries

Wang

Shah

2015

Journal of Molecular and Cellular Cardiology

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“…MMPs, downstream molecules of both Ang II and TGF-β (for reviews) 1, 2 , play causal roles in the development of the aortic aneurysm 59, 68, 69 . MMP-2/-9 activation is able to erode the arterial wall, a histological foundation of the aortic aneurysm development 59, 68 . Further, MMP-2/-9 activation signaling also promotes a loss of VSMCs and facilitates aortic dilation 70 .…”

Section: Arterial Wall Mmp Activation During Aging and In Hypertementioning

confidence: 99%

“…Cathepsin S deficiency decreases MMP-2 activation and retards the pathogenesis of aneurysm 73 . Chronic treatment with a broad-spectrum MMP inhibitor, doxycycline, prevents the development of spontaneous aortic aneurysm lesions 68 .…”

Section: Arterial Wall Mmp Activation During Aging and In Hypertementioning

confidence: 99%

“…The pathophysiological vascular, cellular and molecular events of aging, hypertension, atherosclerosis, and their complications are recapitulated in experimental animals with over-activation of MMPs (Table). In contrast, MMP inhibition attenuates age-associated pathophysiologic arterial remodeling in animal models of hypertension and atherosclerosis 4–8, 68 . Thus, appreciation of the MMP involvement in arterial wall aging and age-associated arterial diseases and the ability to detect its involvement in arterial wall inflammation, vulnerable plaques and the progression of aneurysm/dissection will impact on future translational research to delay arterial remodeling that accompanies aging and its participation in these age-associated arterial diseases.…”

Section: Concluding Remarks and Perspective Viewsmentioning

confidence: 99%

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Matrix Metalloproteinases Promote Arterial Remodeling in Aging, Hypertension, and Atherosclerosis

et al. 2015

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“…13,14 Because the vascular features of these mice do not recapitulate the human disease, we, therefore, decided to induce experimentally vascular dissections or ruptures in young adults Col3a1 +/− and Col3a1 +/+ BALB/c mice, to investigate whether Col3a1 +/− mice are more susceptible to vascular ruptures than wild-type mice as observed in vEDS patients. Among the different experimental methods developed to study the formation and progression of vascular disease, the chronic infusion of angiotensin II (AngII) has consistently been used as a model of aortic dissections and arterial ruptures notably in hypercholesterolemic mice.…”

Section: Col3a1mentioning

confidence: 99%

Angiotensin II Promotes Thoracic Aortic Dissections and Ruptures in Col3a1 Haploinsufficient Mice

Faugeroux

Nematalla²,

Li³

et al. 2013

Hypertension

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Abstract-Vascularmice (73% versus 36%; P=0.03), particularly during the first-week infusion (55% versus 0%). Echocardiography and histological analysis evidenced that early deaths were caused by thoracic aortic ruptures preceded by dissections and associated with low aortic collagen fibrils content. Remarkably, lowering the dose of AngII (0.5 μg/kg per minute) rescued the first-week premature deaths of Col3a1 +/− mice while decreasing the rises in systolic BP (P=0.05 compared with the high-dose AngII), resulting in similar mortality rates in both groups of mice at the end of the 4-week period (30% versus 50% in Col3a1 +/− and Col3a1 +/+ mice; P=0.30). Finally, norepinephrine infusion (3.9 μg/kg per minute) did not induced significant mortality in both groups, whereas it significantly increased systolic BP, comparably with the high and with the low dose of AngII in Col3a1

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Chronic Treatment with a Broad-Spectrum Metalloproteinase Inhibitor, Doxycycline, Prevents the Development of Spontaneous Aortic Lesions in a Mouse Model of Vascular Ehlers-Danlos Syndrome

Cited by 26 publications

References 38 publications

Age-associated pro-inflammatory remodeling and functional phenotype in the heart and large arteries

Age-associated pro-inflammatory remodeling and functional phenotype in the heart and large arteries

Matrix Metalloproteinases Promote Arterial Remodeling in Aging, Hypertension, and Atherosclerosis

Angiotensin II Promotes Thoracic Aortic Dissections and Ruptures in Col3a1 Haploinsufficient Mice

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