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      Dronedarone prevents microcirculatory abnormalities in the left ventricle during atrial tachypacing in pigs

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          Abstract

          BACKGROUND AND PURPOSE

          Atrial fibrillation induces ischaemic microcirculatory flow abnormalities in the ventricle, contributing to the risk for acute coronary syndromes. We evaluated the effect of dronedarone on ventricular perfusion during rapid atrial pacing (RAP).

          EXPERIMENTAL APPROACH

          Coronary and fractional flow reserve (CFR/FFR) were measured in the left anterior descending artery in 29 pigs. Six received RAP, six received RAP with dronedarone (RAP/D), seven received dronedarone alone, four received RAP with amiodarone (RAP/A), and six received neither (sham). In ventricular tissue, oxidative stress/ischaemia-related gene and protein expression was evaluated by RT-PCR and Western blotting; Isoprostanes were measured by GC-MS procedures.

          KEY RESULTS

          CFR was decreased in the RAP group, compared with other groups. FFR was not different between groups. Effective refractory period was reduced in RAP compared with RAP/D. RAP-activated PKC phosphorylation tended to be decreased by dronedarone ( P= 0.055) RAP induced NOX-1 and NOX-2 protein and the mRNA for hypoxia-inducible factor-1α (HIF-1α). Dronedarone reduced the pacing-dependent increase in the expression of NOX-2 protein and of HIF-1α mRNA. The oxidative stress marker, F 2-isoprostane, was increased by RAP and this increase was attenuated by dronedarone. Other oxidative stress/ischaemia-related genes were induced by RAP compared with sham and were decreased by dronedarone treatment. In HL1 cells, dronedarone significantly inhibited the increased phosphorylation of PKCα after oxidative stress, with an almost significant effect ( P= 0.059) on that after RAP.

          CONCLUSIONS AND IMPLICATIONS

          Dronedarone abolished RAP-induced ventricular microcirculatory abnormalities by decreasing oxidative stress/ischaemia-related gene and protein expression in the ventricle.

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          Author and article information

          Journal
          Br J Pharmacol
          Br. J. Pharmacol
          bph
          British Journal of Pharmacology
          Blackwell Publishing Ltd (Oxford, UK )
          0007-1188
          1476-5381
          June 2012
          : 166
          : 3
          : 964-980
          Affiliations
          [1 ] Medical Faculty, Otto von Guericke University Magdeburg, Germany
          [2 ] St. Vincenz-Hospital Paderborn, Germany
          [3 ] Institute of Clinical Chemistry, Department of Pathobiochemistry, Medical Faculty, Otto-von-Guericke University Magdeburg, Germany
          [4 ] Institute of Biometrics, Otto-von-Guericke University Magdeburg, Germany
          [5 ] Department of Medical Biochemistry and Molecular Biology, University of Greifswald Germany
          [6 ] Interfaculty Institute for Genetics and Functional Genomics, Department of Functional Genomics, University of Greifswald Germany
          [7 ] Institute for Pharmacology and preventive Medicine Mahlow, Germany
          Author notes
          Professor Dr Andreas Goette, St. Vincenz-Hospital, Medical Clinic II, Am Busdorf 2, 33098 Paderborn, Germany. E-mail: andreas.goette@ 123456vincenz.de
          Article
          PMC3417422 PMC3417422 3417422
          10.1111/j.1476-5381.2011.01784.x
          3417422
          22103242
          e5b6e1ad-e622-48ff-b69a-1dd2230d4c40
          © 2011 The Authors. British Journal of Pharmacology © 2011 The British Pharmacological Society
          History
          : 15 December 2010
          : 02 November 2011
          : 09 November 2011
          Categories
          Research Papers

          dronedarone,atrial fibrillation,microcirculation,acute coronary syndrome

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