Your search keyword '"Michelakis, Evangelos D."' showing total 3 results

1. Statin therapy, alone or with rapamycin, does not reverse monocrotaline pulmonary arterial hypertension: the rapamcyin-atorvastatin-simvastatin study.

Author

McMurtry, M. Sean, Bonnet, Sebastien, Michelakis, Evangelos D., Bonnet, Sandra, Haromy, Alois, and Archer, Stephen L.

Subjects

HYPERTENSION, PULMONARY artery diseases, SMOOTH muscle, CELL proliferation, RAPAMYCIN, STATINS (Cardiovascular agents), HYPERTROPHY

Abstract

Pulmonary arterial hypertension (PAH) is characterized by excessive pulmonary artery smooth muscle cell proliferation and impaired apoptosis leading to obstruction of resistance pulmonary arteries. We hypothesized that antiproliferative (rapamycin) and proapoptotic (statins) agents, already used clinically for other indications, would decrease experimental PAH, facilitating translation to human therapies. Prior studies in the rat monocrotaline-PAH model have indicated that simvastatin regresses and rapamycin prevents, but cannot reverse, PAH. Two PAH regression strategies (rapamycin monotherapy vs. rapamycin + atorvastatin) and one prevention strategy (simvastatin) were tested in a rat monocrotaline-PAH model. Adult male Sprague-Dawley rats were randomized to saline (n = 6) or monocrotaline (60 mg/kg ip, n = 36) treatment groups. Monocrotaline rats were randomized to gavage with vehicle, rapamycin (2.5 mg·kg-1day-1), or rapamycin + atorvastatin (10 mg·kg-1day-1) treatment groups, beginning 12 days post-monocrotaline. Echocardiographic and hemodynamic end points were assessed 2 wk later. Additional monocrotaline-PAH rats (a = 20) were randomized to vehicle or simvastatin (2 mg·kg-1day-1) treatment groups and followed echocardiographically for 4 wk. Monocrotaline-PAH increased lung p70 S6 kinase phosphorylation, and this was reversed by rapamycin, confirming the biological activity of rapamycin. Despite the use of high doses, neither rapamcyin nor rapamycin + atorvastatin improved survival nor reduced PAH, vascular remodeling, and right ventricular hypertrophy. Although prophylactic simvastatin slowed PAH progression, by 4 wk PAH severity and mortality were not different from placebo. Apart from the new finding of p70 S6 kinase phosphorylation in monocrotaline-PAH, this is a negative therapeutic trial (none of these promising therapies improved monocrotaline-PAH). These negative results should be considered as human trials with these agents are underway (simva-statin) or proposed (rapamycin). [ABSTRACT FROM AUTHOR]

Published

2007

2. Overexpression of human bone morphogenetic protein receptor 2 does not ameliorate monocrotaline pulmonary arterial hypertension.

Author

McMurtry, M. Sean, Moudgil, Rohit, Hashimoto, Kyoko, Bonnet, Sandra, Michelakis, Evangelos D., and Archer, Stephen L.

Subjects

PULMONARY hypertension, HYPERTENSION, PULMONARY circulation, PROTEINS, MONOCROTALINE, APOPTOSIS

Abstract

Pulmonary arterial hypertension (PAH) is associated with mutations of bone morphogenetic protein receptor 2 (BMPR2), and BMPR2 expression decreases with the development of experimental PAH. Decreased BMPR2 expression and impaired intracellular BMP signaling in pulmonary artery (PA) smooth muscle cells (PASMC) suppresses apoptosis and promotes proliferation, thereby contributing to the pathogenesis of PAH. We hypothesized that overexpression of BMPR2 in resistance PAs would ameliorate established monocrotaline PAH. Human BMPR2 was inserted into a serotype 5 adenovirus with a green fluorescent protein (GFP) reporter. Dose-dependent transgene expression was confirmed in PASMC using fluorescence microscopy, quantitative RT-PCR, and immunoblots. PAH was induced by injecting Sprague-Dawley rats with monocrotaline (60 mg/kg ip) or saline. On day 14, post-monocrotaline (MCT) rats received 5 × 109 plaque-forming units of either Ad-human BMPR2 (Ad-hBMPR2) or Ad-GFP. Transgene expression was confirmed by fluorescence microscopy, quantitative RT-PCR of whole lung samples, and laser-capture microdissected resistance PAs. Invasive hemodynamic and echocardiographic end points of pulmonary hypertension were assessed on day 24. Endogenous BMPR2 mRNA levels were greatest in resistance PAs, and expression declined with MCT PAH. Despite robust hBMPR2 expression in all lung lobes and within resistance PAs of treated rats, hBMPR2 did not lower mean PA pressure, pulmonary vascular resistance index, right ventricular hypertrophy, or remodeling of resistance PAs. Nebulized intratracheal adenoviral gene therapy with hBMPR2 reliably distributed hBMPR2 to resistance PAs but did not ameliorate PAH. Depressed BMPR2 expression may be a marker of PAH but is not central to the pathogenesis of this model of PAH. [ABSTRACT FROM AUTHOR]

Published

2007

3. Potassium channels regulate tone in rat pulmonary veins.

Author

Michelakis, Evangelos D., Weir, E. Kenneth, Wu, Xichen, Nsair, Ali, Waite, Ross, Hashimoto, Kyoko, Puttagunta, Lakshmi, Knaus, Hans Gunther, and Archer, Stephen L.

Subjects

*POTASSIUM channels, *PULMONARY veins

Abstract

Presents information on a study which examined whether potassium (K) channels are important in the control of vascular tone in rat intrapulmonary veins. Methodology; Results and discussion.

Published

2001