Ivan M. Rebeyka scite author profile

Background-Sildenafil was recently approved for the treatment of pulmonary arterial hypertension. The beneficial effects of phosphodiesterase type 5 (PDE5) inhibitors in pulmonary arterial hypertension are thought to result from relatively selective vasodilatory and antiproliferative effects on the pulmonary vasculature and, on the basis of early data showing lack of significant PDE5 expression in the normal heart, are thought to spare the myocardium. Methods and Results-We studied surgical specimens from 9 patients and show here for the first time that although PDE5is not expressed in the myocardium of the normal human right ventricle (RV), mRNA and protein are markedly upregulated in hypertrophied RV (RVH) myocardium. PDE5 also is upregulated in rat RVH. PDE5 inhibition (with either MY-5445 or sildenafil) significantly increases contractility, measured in the perfused heart (modified Langendorff preparation) and isolated cardiomyocytes, in RVH but not normal RV. PDE5 inhibition leads to increases in both cGMP and cAMP in RVH but not normal RV. Protein kinase G activity is suppressed in RVH, explaining why the PDE5 inhibitor-induced increase in cGMP does not lead to inhibition of contractility. Rather, it leads to inhibition of the cGMP-sensitive PDE3, explaining the increase in cAMP and contractility. This is further supported by our findings that, in RVH protein kinase A, inhibition completely inhibits PDE5-induced inotropy, whereas protein kinase G inhibition does not. Conclusions-The ability of PDE5 inhibitors to increase RV inotropy and to decrease RV afterload without significantly affecting systemic hemodynamics makes them ideal for the treatment of diseases affecting the RV, including pulmonary arterial hypertension. (Circulation. 2007;116:238-248.)

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ABO-Incompatible Heart Transplantation in Infants

West

et al. 2001

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Risk Factors for and Outcomes of Acute Kidney Injury in Neonates Undergoing Complex Cardiac Surgery

Morgan

Zappitelli

Robertson

et al. 2013

The Journal of Pediatrics

235

185

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Scimitar syndrome: Twenty years' experience and results of repair

Najm¹,

Williams²,

Coles³

et al. 1996

The Journal of Thoracic and Cardiovascular Surgery

180

178

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Oxygen Activates the Rho/Rho-Kinase Pathway and Induces RhoB and ROCK-1 Expression in Human and Rabbit Ductus Arteriosus by Increasing Mitochondria-Derived Reactive Oxygen Species

et al. 2007

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Background-Constriction of the ductus arteriosus (DA) is initiated at birth by inhibition of O 2 -sensitive K ϩ channels in DA smooth muscle cells. Subsequent membrane depolarization and calcium influx through L-type calcium channels initiates functional closure. We hypothesize that Rho-kinase activation is an additional mechanism that sustains DA constriction. Methods and Results-The effect of increased PO 2 on the activity and expression of Rho-kinase was assessed in DAs from neonates with hypoplastic left-heart syndrome (nϭ15) and rabbits (339 term and 99 preterm rabbits). Rho-kinase inhibitors (Y-27632 and fasudil) prevent and reverse O 2 constriction. Heterogeneity exists in the sensitivity of constrictors (PO 2 ϭendothelinϭphenylephrineϾKCl) and of fetal vessels (DAϭpulmonary arteryϾaorta) to Rho-kinase inhibition. Inhibition of L-type calcium channels (nifedipine) or removal of extracellular calcium inhibits approximately two thirds of O 2 constriction. Residual DA constriction reflects calcium sensitization, which persists after removal of extracellular calcium and blocking of sarcoplasmic reticulum Ca 2ϩ -ATPase. In term DA, an increase in PO 2 activates Rho-kinase and thereby increases RhoB and ROCK-1 expression. Activation of Rho-kinase in DA smooth muscle cells is initiated by a PO 2 -dependent, rotenone-sensitive increase in mitochondrion-derived reactive O 2 species. O 2 effects on Rho-kinase are mimicked by exogenous H 2 O 2 . In preterm DAs, immaturity of mitochondrial reactive oxygen species generation is associated with reduced and delayed O 2 constriction and lack of PO 2 -dependent upregulation of Rho-kinase expression. Conclusions-O 2 activates Rho-kinase and increases Rho-kinase expression in term DA smooth muscle cells by a redox-regulated, positive-feedback mechanism that promotes sustained vasoconstriction. Conversely, Rho-kinase inhibitors may be useful in maintaining DA patency, as a bridge to congenital heart surgery.

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Ivan M. Rebeyka

Phosphodiesterase Type 5 Is Highly Expressed in the Hypertrophied Human Right Ventricle, and Acute Inhibition of Phosphodiesterase Type 5 Improves Contractility

ABO-Incompatible Heart Transplantation in Infants

Risk Factors for and Outcomes of Acute Kidney Injury in Neonates Undergoing Complex Cardiac Surgery

Scimitar syndrome: Twenty years' experience and results of repair

Oxygen Activates the Rho/Rho-Kinase Pathway and Induces RhoB and ROCK-1 Expression in Human and Rabbit Ductus Arteriosus by Increasing Mitochondria-Derived Reactive Oxygen Species

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