Chronic pulmonary hypertension‐the monocrotaline model and involvement of the hemostatic system

Schultze, A. Eric; Roth, Robert A.

doi:10.1080/10937409809524557

Cited by 93 publications

(75 citation statements)

References 263 publications

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“…Closed-chest right-and left-heart microcardiac catheterization in live animals detected pulmonary hypertension in all sickle mice studied but not in hemizygous colony controls or wild-type controls. The pulmonary hypertension occurred spontaneously, unlike the need for experimental triggers in other animal models, [33][34][35][36] and without evidence of thrombosis or major vascular remodeling. The pulmonary hypertension was mediated by a functional impairment in endothelial-dependent vasodilation, NO resistance, and increased vasoconstrictor tone.…”

Section: Introductionmentioning

confidence: 85%

Hemolysis in sickle cell mice causes pulmonary hypertension due to global impairment in nitric oxide bioavailability

Hsu

Champion

Campbell‐Lee

et al. 2006

Blood

227

208

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Pulmonary hypertension is a highly prevalent complication of sickle cell disease and is a strong risk factor for early mortality. However, the pathophysiologic mechanisms leading to pulmonary vasculopathy remain unclear. Transgenic mice provide opportunities for mechanistic studies of vascular pathophysiology in an animal model. By microcardiac catheterization, all mice expressing exclusively human sickle hemoglobin had pulmonary hypertension, profound pulmonary and systemic endothelial dysfunction, and vascular instability characterized by diminished responses to authentic nitric oxide (NO), NO donors, and endothelium-dependent vasodilators and enhanced responses to vasoconstrictors. However, endothelium-independent vasodilation in sickle mice was normal. Mechanisms of vasculopathy in sickle mice involve global dysregulation of the NO axis: impaired constitutive nitric oxide synthase activity (NOS) with loss of endothelial NOS (eNOS) dimerization, increased NO scavenging by plasma hemoglobin and superoxide, increased arginase activity, and depleted intravascular nitrite reserves. Light microscopy and computed tomography revealed no plexogenic arterial remodeling or thrombi/ emboli. Transplanting sickle marrow into wild-type mice conferred the same phenotype, and similar pathobiology was observed in a nonsickle mouse model of acute alloimmune hemolysis. Although the time course is shorter than typical pulmonary hypertension in human sickle cell disease, these results demonstrate that hemolytic anemia is sufficient to produce endothelial dysfunction and global dysregulation of NO. IntroductionPulmonary hypertension is a highly prevalent complication of sickle cell disease that is associated with early mortality. [1][2][3][4] The putative mechanisms responsible for pulmonary hypertension are the focus of intense current research and remain incompletely defined. 5 One mechanism proposed is that hemolytic anemia and decompartmentalization of erythrocyte hemoglobin and arginase into plasma leads to nitric oxide (NO) scavenging and arginine degradation, limiting the bioavailability of NO. 3,[6][7][8][9][10] This process would ultimately lead to acute changes in pulmonary vascular endothelial and vasomotor function and chronic pathologic intimal and smooth muscle hyperplasia. Alternatively, chronic lung disease caused by recurrent pulmonary infarction, pneumonia, acute chest syndrome, and thromboembolism could lead to chronic hypoxemia, pulmonary fibrosis, thrombotic vascular obliteration, and secondary pulmonary hypertension. [11][12][13][14][15] Pulmonary hypertension could also arise from chronic hypoxia or chronic nocturnal hypoxia. [16][17][18] Additional factors contributing to pulmonary hypertension include right-heart failure secondary to a chronic high cardiac output as compensation for chronic anemia and left ventricular diastolic dysfunction secondary to cardiac tissue microinfarction and/or iron overload. [19][20][21][22] In short, is exposure to hemoglobin S (HbS) erythrocytes sufficient to cause pulmonar...

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Section: Introductionmentioning

confidence: 85%

Hemolysis in sickle cell mice causes pulmonary hypertension due to global impairment in nitric oxide bioavailability

Hsu

Champion

Campbell‐Lee

et al. 2006

Blood

227

208

View full text Add to dashboard Cite

show abstract

“…A rise in pulmonary artery hypertension induces right ventricular hypertrophy and right ventricular failure and eventually leads to premature death. It is well known that a single subcutaneous administration of the pyrrolizidine alkaloid monocrotaline to rats causes cardiovascular and pulmonary disorders similar to those seen in patients with pulmonary artery hypertension (1,2), including severe right ventricular hypertrophy (3,4) and right ventricular failure (5 -8). Despite extensive studies, the fundamental mechanisms responsible for the development and progression of right ventricular failure have not been fully elucidated.…”

Section: Introductionmentioning

confidence: 99%

Possible Involvement of Mitochondrial Energy-Producing Ability in the Development of Right Ventricular Failure in Monocrotaline-Induced Pulmonary Hypertensive Rats

et al. 2009

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Abstract. The present study was undertaken to explore the possible involvement of alterations in the mitochondrial energy-producing ability in the development of the right ventricular failure in monocrotaline-administered rats. The rats at the 6th week after subcutaneous injection of 60 mg/kg monocrotaline revealed marked myocardial hypertrophy and fibrosis, that is, severe cardiac remodeling. The time-course study on the cardiac hemodynamics of the monocrotalineadministered rat by the cannula and echocardiographic methods showed a reduction in cardiac double product, a decrease in cardiac output index, and an increase in the right ventricular Tei index, suggesting that the right ventricular failure was induced at the 6th week after monocrotaline administration in rats. The mitochondrial oxygen consumption rate of the right ventricular muscle isolated from the monocrotaline-administered animal was decreased, which was associated with a reduction in myocardial high-energy phosphates. Furthermore, the decrease in mitochondrial oxygen consumption rate was inversely related to the increase in the right ventricular Tei index of the monocrotaline-administered rats. These results suggest that impairment of the mitochondrial energy-producing ability is involved in the development of the right ventricular failure in monocrotaline-induced pulmonary hypertensive rats.

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“…This is of importance because different levels of growlh factors and their receptors can modulate/activate the HIF pathway through stimulation of phosphorylation cascades. The three broad subfamilies of the mitogen-activated protein kinase (MAPK) cascades, namely the c-Jun NHj-terminal kinases (JNKs), p38 MAPKs and the extracellular signal-regulated kinases (Erks) have been shown to be involved in the regulation of the HIF-pathway (2,41,109,118,135). Interestingly, although HIF-la is a highly phosphorylated protein and two Erkl/Erk2 MAPK consensus sites (PXSP) ex-ist on the human HIF-1 a (positions 515 and 687), point mutations did not reveal the exact phosphorylation sites (118).…”

Section: Hif-la Phosphorylation -Regulation Of Hif-1 By External Stimulimentioning

confidence: 99%

International Hypoxia Symposium (13th) for the Publishing of the Conference Proceedings for 2003 Conference

Roach¹,

Hackett²,

Wagner³

2004

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Chronic pulmonary hypertension‐the monocrotaline model and involvement of the hemostatic system

Cited by 93 publications

References 263 publications

Hemolysis in sickle cell mice causes pulmonary hypertension due to global impairment in nitric oxide bioavailability

Hemolysis in sickle cell mice causes pulmonary hypertension due to global impairment in nitric oxide bioavailability

Possible Involvement of Mitochondrial Energy-Producing Ability in the Development of Right Ventricular Failure in Monocrotaline-Induced Pulmonary Hypertensive Rats

International Hypoxia Symposium (13th) for the Publishing of the Conference Proceedings for 2003 Conference

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