Important role of tissue angiotensin-converting enzyme activity in the pathogenesis of coronary vascular and myocardial structural changes induced by long-term blockade of nitric oxide synthesis in rats.

Takemoto, Masao; Egashira, Kensuke; Usui, Makoto; Numaguchi, Kohtaro; Tomita, Hideharu; Tsutsui, Hiroyuki; Shimokawa, Hiroaki; Sueishi, Katsuo; Takeshita, Akira

doi:10.1172/jci119156

Cited by 313 publications

(258 citation statements)

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“…4,5 The structural changes consistently observed after long-term NOS inhibition include vascular hypertrophy and adventitial collagen deposition. 6 A number of factors may contribute to this pathology, including increased local vascular expression of ACE, 6 endothelin production, 7 and the induction of type I collagen expression. 8 Conversely, ACE inhibition and endothelin antagonists have been shown to prevent hypertension and perivascular fibrosis in L-NAMEtreated animals.…”

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confidence: 99%

“…8 Conversely, ACE inhibition and endothelin antagonists have been shown to prevent hypertension and perivascular fibrosis in L-NAMEtreated animals. 6,8 Aside from the well-defined roles that endothelial NO plays in regulating vascular tone and structure, it has also been reported that NO suppresses plasminogen activator inhibitor-1 (PAI-1) expression in vascular tissue. 9 It was recently reported that long-term NOS inhibition induced vascular PAI-1 expression in rat models.…”

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confidence: 99%

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Plasminogen Activator Inhibitor-1 Deficiency Prevents Hypertension and Vascular Fibrosis in Response to Long-term Nitric Oxide Synthase Inhibition

et al. 2001

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Background-Long-term inhibition of nitric oxide synthase (NOS) is known to induce hypertension and perivascular fibrosis. Recent evidence also suggests that long-term NOS inhibition induces expression of plasminogen activator inhibitor-1 (PAI-1) in vascular tissues and that PAI-1 may contribute to the development of fibrosis after chemical or ionizing injury. On the basis of these observations, we hypothesized that PAI-1 may influence the vascular response to long-term NOS inhibition by N -nitro-L-arginine methyl ester (L-NAME). Methods and Results-We compared the temporal changes in systolic blood pressure and coronary perivascular fibrosis in PAI-1-deficient (PAI-1 Ϫ/Ϫ ) and wild-type (WT) male mice (Nϭ6 per group). At baseline, there were no significant differences in blood pressure between groups. After initiation of L-NAME, systolic blood pressure increased in both groups at 2 weeks. Over an 8-week study period, systolic blood pressure increased to 141Ϯ3 mm Hg in WT animals versus 112Ϯ4 mm Hg in PAI-1 Ϫ/Ϫ mice (PϽ0.0001). The extent of coronary perivascular fibrosis increased significantly in L-NAME-treated WT mice (PϽ0.01 versus PAI-1 Ϫ/Ϫ mice). Cardiac type I collagen mRNA expression was greater in control (PϽ0.01) and L-NAME-treated PAI-1 Ϫ/Ϫ (PϽ0.05) groups than in control WT mice, indicating that PAI-1 deficiency prevents the increase of collagen deposition by promoting matrix degradation. Conclusions-These findings suggest that PAI-1 deficiency alone is sufficient to protect against the structural vascular changes that accompany hypertension in the setting of long-term NOS inhibition. Direct inhibition of vascular PAI-1 activity may provide a new therapeutic strategy for the prevention of arteriosclerotic cardiovascular disease.

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confidence: 99%

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confidence: 99%

Plasminogen Activator Inhibitor-1 Deficiency Prevents Hypertension and Vascular Fibrosis in Response to Long-term Nitric Oxide Synthase Inhibition

et al. 2001

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“…These data on the ability of taxifolin to bring the ACE activity to the normal level have been obtained for the first time; however, it is possible to compare them with the influence of flavonoids on other manifestations of age-related vessel pathology or pathology caused by the NO synthase inhibitor or glucocorticoid hormones. As known, vessel remodeling in rats enhances with aging (Basso et al 2007) and as a result of the effect of the NO synthase inhibitor (Takemoto et al 1997;Katoh et al 2001). In these cases, pathological changes in vessels are caused by enhanced ACE activity because ACE inhibitors prevent vessel remodeling (Takemoto et al 1997;Katoh et al 2001;Basso et al 2007).…”

Section: Discussionmentioning

confidence: 99%

“…As known, vessel remodeling in rats enhances with aging (Basso et al 2007) and as a result of the effect of the NO synthase inhibitor (Takemoto et al 1997;Katoh et al 2001). In these cases, pathological changes in vessels are caused by enhanced ACE activity because ACE inhibitors prevent vessel remodeling (Takemoto et al 1997;Katoh et al 2001;Basso et al 2007). Glucocorticoid hormones also increase the ACE activity in the aorta ), blood pressure (Saruta 1996), and the risk of CVD (Nashel 1986;Souverein et al 2004).…”

Section: Discussionmentioning

confidence: 99%

“…Both types of cells contain a significant amount of active (intranuclear) 5-lipoxygenase (Mehrabian and Allayee 2003). The increase in the contribution of NADPH oxidase is caused by its activation by angiotensin II (Griendling et al 1994;Rajagopalan et al 1996;Landmesser et al 2002), the concentration of which rises upon treatment of rats with L-NAME because of the increase in the ACE activity (Takemoto et al 1997;Korystova et al 2012). There are data showing that the activation of NADPH oxidase with angiotensin II depends on 5-lipoxygenase: angiotensin II activates 5-lipoxygenase and LTB4, a product of 5-lipoxygenase, activates NADPH oxidase (Luchtefeld et al 2003).…”

Section: Discussionmentioning

confidence: 99%

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Effects of taxifolin on the activity of angiotensin-converting enzyme and reactive oxygen and nitrogen species in the aorta of aging rats and rats treated with the nitric oxide synthase inhibitor and dexamethasone

Arutyunyan

Korystova

Kublik

et al. 2012

AGE

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The action of taxifolin on the angiotensinconverting enzyme (ACE) and the formation of reactive oxygen and nitrogen species (ROS/RNS) in the aorta of aging rats and rats treated with nitric oxide synthase inhibitor (N ω -nitro-L-arginine methyl ester (L-NAME)) or dexamethasone have been studied. The ACE activity in aorta sections was determined by measuring the hydrolysis of hippuryl-L-histidyl-L-leucine, and the ROS/ RNS production was measured by oxidation of dichlorodihydrofluorescein. It was shown that taxifolin at a dose of 30-100 μg/kg/day decreases the ACE activity in the aorta of aging rats and of rats treated with L-NAME or dexamethasone to the level of the ACE activity in young control rats. Taxifolin (100 μg/kg/day) was found to also reduce the amount of ROS/RNS in the aorta that increased as a result of L-NAME intake. L-NAME treatment increases the contribution of 5-lipoxygenase and NADPH oxidase to ROS/RNS production in the aorta, while taxifolin (100 μg/kg/day) decreases the contribution of these enzymes to the normal level.

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Vasculoprotective and Cardioprotective Mechanisms of Angiotensin‐Converting Enzyme Inhibition: The Homeostatic Balance Between Angiotensin II and Nitric Oxide

Gibbons

1997

Clinical Cardiology

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The ability of the vasculature to modify its geometry in accordance with conditions of its microenvironment—the process of vascular remodeling—is an important pathobiologic process common to vascular disorders such as atherosclerosis, restenosis after angioplasty, and hypertension. Vascular remodeling characterizes the natural history of atherosclerosis, contributes to increased vascular resistance, and may contribute to the clinical complications of hypertension. A growing body of evidence indicates that locally generated vasoactive substances such as angiotensin II and nitric oxide are important determinants of the natural history of vascular disease. In particular, angiotensin II may promote vascular lesion formation by increasing vascular cell population via increased cell growth and decreased programmed cell death, and it may also alter extracellular matrix composition. Thus, angiotensin II is a pleiotropic local mediator capable of modulating cell growth, programmed cell death, migration of vascular smooth muscle cells, and extracellular matrix modulation, all of which are biologic mechanisms of vascular remodeling and intimal formation. This is proposed to occur via a local tissue angiotensin system. Angiotensin II may also promote chronic hypertension by modulating the vascular redox state and promoting the catabolism of the endothelium‐derived nitric oxide, an endogenous inhibitory vasodilator. Because angiotensin‐converting enzyme (ACE) is strategically positioned to influence the activity of at least three local vasoactive systems—angiotensin II, nitric oxide, and bradykinin—blocking ACE with ACE inhibition may have profound effects on ventricular and vascular structure and function, and have particular efficacy in preventing the morbidity and mortality of vascular diseases such as hypertension and atherosclerosis.

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Important role of tissue angiotensin-converting enzyme activity in the pathogenesis of coronary vascular and myocardial structural changes induced by long-term blockade of nitric oxide synthesis in rats.

Cited by 313 publications

References 42 publications

Plasminogen Activator Inhibitor-1 Deficiency Prevents Hypertension and Vascular Fibrosis in Response to Long-term Nitric Oxide Synthase Inhibition

Plasminogen Activator Inhibitor-1 Deficiency Prevents Hypertension and Vascular Fibrosis in Response to Long-term Nitric Oxide Synthase Inhibition

Effects of taxifolin on the activity of angiotensin-converting enzyme and reactive oxygen and nitrogen species in the aorta of aging rats and rats treated with the nitric oxide synthase inhibitor and dexamethasone

Vasculoprotective and Cardioprotective Mechanisms of Angiotensin‐Converting Enzyme Inhibition: The Homeostatic Balance Between Angiotensin II and Nitric Oxide

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