Mechanisms Involved in Cardioprotective Effects of Pravastatin Administered during Reoxygenation in Human Myocardium In Vitro-Reference-Cited by-同舟云学术

Mechanisms Involved in Cardioprotective Effects of Pravastatin Administered during Reoxygenation in Human Myocardium In Vitro

Published:2012-04-01 Issue:4 Volume:116 Page:824-833
ISSN:0003-3022
Container-title:Anesthesiology
language:en
Short-container-title:

Author:

Lemoine Sandrine¹,Allouche Stéphane²,Coulbault Laurent³,Cornet Valérie⁴,Massetti Massimo⁵,Galera Philippe⁶,Gérard Jean-Louis⁷,Hanouz Jean-Luc⁸

Affiliation:

1. Postdoctoral Fellow, Laboratory of Experimental Anesthesiology and Cellular Physiology EA3212.

2. Associate Professor of Biochemistry, Faculty of Medicine, Centre Hospitalier Universitaire de Caen, France, Laboratory of Molecular and Cellular Biology of Signalling, UPRES EA3919.

3. Associate Professor of Pharmacology, Faculty of Medicine, Centre Hospitalier Universitaire de Caen, France, Laboratory of Molecular and Cellular Biology of Signalling, UPRES EA3919.

4. Post Graduate Student, Laboratory of Experimental Anesthesiology and Cellular Physiology EA3212.

5. Professor of Cardiac Surgery, Department of Cardiac and Surgery.

6. Professor of Molecular Biology, Laboratory of Extracullar Matrice and Pathology, EA3214, IFR ICORE146, Université de Caen Basse Normandie, Caen, France.

7. Professor of Anesthesiology, Department of Anesthesiology.

8. Professor of Anesthesiology, Chairman, Director of the Laboratory of Experimental Anesthesiology and Cellular Physiology EA3212, Department of Anesthesiology, Centre Hospitalier Universitaire de Caen, Caen, France.

Abstract

Background The authors investigated the effect of pravastatin during reoxygenation after myocardial hypoxia and examined the involvement of nitric oxide synthase, mitochondrial permeability transition pore, and expression of markers of apoptosis in human myocardium in vitro. Methods Human atrial trabeculae were exposed to hypoxia for 30 min and reoxygenation for 60 min (control group; n = 10). Pravastatin (5, 10, 50, 75 μM; n = 6 in each group) was administered throughout the reoxygenation. In separate groups (n = 6 in each group), pravastatin 50 μM was administered in the presence of 200 μM L-NG-nitroarginine methyl ester, a nitric oxide synthase inhibitor, and 50 μM atractyloside, the mitochondrial permeability transition pore opener. The primary endpoint was the developed force of contraction at the end of reoxygenation, expressed as a percentage of baseline (mean ± SD). Protein expression of BAD, phospho-BAD, caspase 3, Pim-1 kinase, and Bcl-2 were measured using Western immunoblotting. Results The administration of 10 (77 ± 5% of baseline), 50 (86 ± 6%), and 75 μM (88 ± 13%) pravastatin improved the force of contraction at the end of reoxygenation, compared with that of the control group (49 ± 11%; P < 0.001). These beneficial effects were prevented by L-NG-nitroarginine methyl ester and atractyloside. Compared with control group, the administration of 5 μM pravastatin did not modify the force of contraction. Pravastatin increased the phosphorylation of BAD, activated the expression of Pim-1 kinase and Bcl-2, and maintained the caspase 3 concentration relative to that of the respective untreated controls. Conclusions Pravastatin, administered at reoxygenation, protected the human myocardium by preventing the mitochondrial permeability transition pore opening, phosphorylating BAD, activating nitric oxide synthase, Pim-1 kinase, and Bcl-2, and preserving the myocardium against the caspase 3 activation.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Anesthesiology and Pain Medicine

Link

http://pubs.asahq.org/anesthesiology/article-pdf/116/4/824/257007/00000542-201204000-00017.pdf

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