Smooth Muscle Apoptosis During Vascular Regression in Spontaneously Hypertensive Rats

deBlois, Denis; Tea, Bun-Seng; Dam, Than‐Vinh; Tremblay, Johanne; Hamet, Pavel

doi:10.1161/01.hyp.29.1.340

Cited by 156 publications

(154 citation statements)

References 71 publications

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“…Previous evidence supporting an early remodeling process has shown in aorta that there is a "burst" of vascular smooth muscle cell apoptosis within the first 2 weeks of antihypertensive treatment. 30,31 Regardless of the precise mechanism of remodeling, the present findings describe a time course of vascular structural changes that occur during both the on-and the off-treatment time periods. Specifically, changes in the index of lumen dimensions were not fully consolidated until 2 to 3 weeks after stopping treatment.…”

Section: Discussionmentioning

confidence: 72%

Time Course of Vascular Structural Changes During and After Short-Term Antihypertensive Treatment

et al. 2003

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Abstract-The present study characterized the persistent changes (ie, off-treatment) resulting from short-term antihypertensive treatments on mean arterial pressure (MAP) and structurally based vascular resistance. Rats were treated for 14 days with enalapril (30 mg · kg Ϫ1 · d Ϫ1 ) with regular (ENAL, 0.4%) or low salt (ELS, 0.04%) diets, or a triple therapy (Triple: hydralazine 45 mg · kg Ϫ1 · d Ϫ1

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Section: Discussionmentioning

confidence: 72%

Time Course of Vascular Structural Changes During and After Short-Term Antihypertensive Treatment

et al. 2003

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“…Smooth muscle and endothelial cell apoptosis have been shown to play an important role in vascular regression in physiological and pathological processes (Bennet and Boyle, 1998;deBlois et al, 1997;Goede et al, 1998;Honma and Hamasaki, 1998;Modlich et al, 1996;Shabisgh et al, 1999;Walker and Gobe, 1987;Walker et al, 1989). For example, there is increasing evidence showing that vascular smooth muscle cell apoptosis is involved in the pathogenesis of atherosclerosis and restenosis following angioplasty (Bennet and Boyle, 1998).…”

Section: Vascular Involution Is An Important Step In the Chain Of Evementioning

confidence: 99%

Vascular Apoptosis and Involution in Gliomas Precede Neovascularization: A Novel Concept for Glioma Growth and Angiogenesis

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Amirnovin

Greco

et al. 2000

Laboratory Investigation

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SUMMARY:Vascular changes in gliomas were analyzed by implanting fluorescent-labeled glioma 261 cells in the brains of 28 mice. Seven animals were killed each week for 4 weeks. We investigated the expression of angiopoietin-2 (Ang-2) by in situ hybridization and compared it with the distribution of apoptotic cells identified by DNA strand breaks (using the terminal deoxynucleotidyl transferase-mediated biotinylated deoxyuridine triphosphate nick end labeling [TUNEL] method) and transmission electron microscopy (TEM). As early as 1 week after implantation, tumor cells accumulated around vessels, which expressed Ang-2 and were TUNEL negative. TEM showed tumor cells adjacent to the vascular cells "lifting up" the normal astrocytic feet processes away from the endothelial cells and disrupting normal pericytic cuffing. After 2 weeks the number of perivascular glioma cells had increased. No increase in the number of blood vessels was detected at this time. Vascular cells remained positive for Ang-2 and rare ones were TUNEL positive. TEM showed closely packed proliferating perivascular tumor cells. After 3 weeks, there was vascular involution with scant zones of tumor necrosis. Ang-2 was still detected in vascular cells, but now numerous vascular cells were TUNEL positive. In addition, TEM showed apoptotic vascular cells. After 4 weeks, there were extensive areas of tumor necrosis with pseudopalisading and adjacent angiogenesis. Ang-2 was detected in vascular cells at the edge of the tumors in the invaded brain and in vessels surrounded by tumor cells. At both 3 and 4 weeks, most of the TUNEL-positive tumor cells lacked morphological features characteristic of apoptosis and displayed features consistent with necrotic cell death as determined by TEM. Only rare tumor cells appeared truly apoptotic. In contrast, the TUNEL-positive endothelial cells and pericytes were round and shrunken, with condensed nuclear chromatin by TEM, suggesting that vascular cells were undergoing an apoptotic cell death. These results suggest that vascular cell apoptosis and involution preceded tumor necrosis and that angiogenesis is a later event in tumor progression in experimental gliomas. Moreover, Ang-2 is detected prior to the onset of apoptosis in vascular cells and could be linked to vascular involution. (Lab Invest 2000, 80:837-849).A poptosis and angiogenesis are both critical events in the normal sequences of many biologic processes and play key roles in regulatory activities during normal and pathological processes including development and oncogenesis. Apoptosis and angiogenesis are as fundamental to cellular and tissue physiology as are cell division and differentiation. In contrast to necrosis, apoptosis may affect scattered individual cells rather than clusters of cells, entire tissues, or organ compartments (Majno and Joris, 1995). One of the key characteristics of apoptosis is cell shrinkage. Apoptosis represents a mechanism to remove damaged, infected, or unwanted cells selectively (Allen et al, 1998;Dinsdale et al, 1999;Payne ...

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“…Certain antihypertensive drugs have been shown to provide long-term benefits beyond blood pressure lowering. For example, angiotensin converting enzyme (ACE) inhibitors have been shown clinically 2 and experimentally, 3,4 to reduce cardiovascular mortality, in part by decreasing cardiac and vascular hypertrophy 5 as well as cardiac and renal fibrosis. [6][7][8] We have previously demonstrated in experimental models of hypertension that ACE inhibitor-induced regression of cardiac hypertrophy is mediated in part by apoptosis of fibroblasts in addition to reduction in cardiomyocyte size in the left ventricle (LV).…”

Section: Introductionmentioning

confidence: 99%

Short-term ACE inhibition confers long-term protection against target organ damage

et al. 2012

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Angiotensin converting enzyme (ACE) inhibitors reduce left ventricular (LV) hypertrophy and cardiovascular-renal fibrosis. Experimentally, changes in the LV and kidney persist even after cessation of treatment. The present study investigates whether brief ACE inhibition in spontaneously hypertensive rats (SHR) provides long-term protection against the LV and kidney damage induced by the nitric oxide synthase inhibitor N-x-nitro-L-arginine-methyl ester (L-NAME). SHR received the ACE inhibitor enalapril (n¼36) or tap water (n¼36). In all, 12 control and treated SHR were sacrificed after 2 weeks and remaining rats were taken off-treatment. After a 2-week washout, 12 controls or previously treated SHR were sacrificed and remaining rats were treated with L-NAME ((control (Con)+L, enalapril (Enal)+L) for 10 days. At sacrifice, blood pressure was recorded via carotid artery cannulation in anesthetized rats, and blood, the kidney and LV were isolated for analysis. LV mass and arterial pressure were significantly reduced by enalapril. LV mass showed a persistent reduction throughout the study. In LV, prior enalapril treatment provided significant (Po0.05) protection against L-NAME-induced increases in proliferating cells (Con+L: 11±10.0 mm 2 vs. Enal+L: 4±4.4 mm 2 ), interstitial fibrosis (Con+L: 3±2.5% vs. Enal+L: 1±1.0%) and tissue macrophages (Con+L: 12±9 mm 2 vs. Enal+L: 5±3.6 mm 2 ). In the kidney, prior enalapril treatment protected against L-NAME-induced interstitial fibrosis and vascular injury. There was no difference in glomerular size or glomerulosclerosis regardless of prior treatment. Plasma creatinine and urea were significantly increased in L-NAME treated rats. This study suggests that brief ACE inhibition confers protection against future heart and kidney injury, even in the absence of continued antihypertensive treatment.

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Smooth Muscle Apoptosis During Vascular Regression in Spontaneously Hypertensive Rats

Cited by 156 publications

References 71 publications

Time Course of Vascular Structural Changes During and After Short-Term Antihypertensive Treatment

Time Course of Vascular Structural Changes During and After Short-Term Antihypertensive Treatment

Vascular Apoptosis and Involution in Gliomas Precede Neovascularization: A Novel Concept for Glioma Growth and Angiogenesis

Short-term ACE inhibition confers long-term protection against target organ damage

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