DOI: 10.1159/000416017
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Effect of Treatment with Recombinant Human Erythropoietin on Peripheral Hemodynamics and Oxygenation

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Cited by 67 publications
(31 citation statements)
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“…When stimulated by vasoactive agents such as acetylcholine or by increased shear stress, mechanism by which TPR may increase with correction of the anemia is via the reversal of hypoxic vasodilatation endothelial cells produce an endothelial factor identified as nitric oxide (NO). The release of endogenous NO from following improved tissue oxygenation [31]. The observation that EPO therapy can induce hypertension without endothelial cells tonically reduces the peripheral vascular resistance and BP.…”
Section: Arginine Vasopressin Erythropoietinmentioning
confidence: 99%
“…When stimulated by vasoactive agents such as acetylcholine or by increased shear stress, mechanism by which TPR may increase with correction of the anemia is via the reversal of hypoxic vasodilatation endothelial cells produce an endothelial factor identified as nitric oxide (NO). The release of endogenous NO from following improved tissue oxygenation [31]. The observation that EPO therapy can induce hypertension without endothelial cells tonically reduces the peripheral vascular resistance and BP.…”
Section: Arginine Vasopressin Erythropoietinmentioning
confidence: 99%
“…It had been proposed that tissue protection and repair associated with EPO depends upon a heteromeric receptor composed of EPO receptor subunits complexed with the beta common receptor (CD131) also used by other type I cytokines, resulting in activation of a whole array of antiapoptotic and antiinflammatory pathways (Brines et al, 2004). However, due to its erythropoietic potency, which has made EPO so useful for treatment of anemia, and due to increased risk of thrombosis (Wolf et al, 1997a,b;Stohlawetz et al, 2000;Haiden et al, 2005;Stasko et al, 2007;Kirkeby et al, 2008;Kato et al, 2010) and hypertension (Nonnast-Daniel et al, 1988;Schaefer et al, 1988;Vaziri, 1999), continuous EPO administration is unacceptable for treatment of CHF. Even a single dose of recombinant human EPO (rhEPO), in fact, can be associated with undesirable increases in platelet activation and number (Lippi et al, 2010).…”
Section: Introductionmentioning
confidence: 99%
“…Major putative mechanisms for the increase in blood pressure by repeated rHuEPO administration are expansion of blood volume, increased blood viscosity (4), and reversal of hypoxic vasodilatation (5). A direct vasoconstrictive effect of rHuEPO was also inferred from the results of an in vitro animal study in which vascular smooth muscle cells constricted in response to high concentrations of rHuEPO (10-200 U/ml) (6).…”
Section: Introductionmentioning
confidence: 99%