Universität Münster
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Intravenous sphingosylphosphorylcholine protects ischemic and postischemic myocardial tissue in a mouse model of myocardial ischemia/reperfusion injury.

Herzog C, Schmitz M, Levkau B, Herrgott I, Mersmann J, Larmann J, Johanning K, Winterhalter M, Chun J, Müller FU, Echtermeyer F, Hildebrand R, Theilmeier G

Forschungsartikel (Zeitschrift)

Zusammenfassung

HDL, through sphingosine-1-phosphate (S1P), exerts direct cardioprotective effects on ischemic myocardium. It remains unclear whether other HDL-associated sphingophospholipids have similar effects. We therefore examined if HDL-associated sphingosylphosphorylcholine (SPC) reduces infarct size in a mouse model of transient myocardial ischemia/reperfusion. Intravenously administered SPC dose-dependently reduced infarct size after 30 minutes of myocardial ischemia and 24 hours reperfusion compared to controls. Infarct size was also reduced by postischemic, therapeutical administration of SPC. Immunohistochemistry revealed reduced polymorphonuclear neutrophil recruitment to the infarcted area after SPC treatment, and apoptosis was attenuated as measured by TUNEL. In vitro, SPC inhibited leukocyte adhesion to TNF?-activated endothelial cells and protected rat neonatal cardiomyocytes from apoptosis. S1P(3) was identified as the lysophospholipid receptor mediating the cardioprotection by SPC, since its effect was completely absent in S1P(3)-deficient mice. We conclude that HDL-associated SPC directly protects against myocardial reperfusion injury in vivo via the S1P(3) receptor.

Details zur Publikation

FachzeitschriftMediators of Inflammation (Mediators Inflamm)
Jahrgang / Bandnr. / Volume2010
StatusVeröffentlicht
Veröffentlichungsjahr2010
Sprache, in der die Publikation verfasst istEnglisch

Autor*innen der Universität Münster

Herrgott, Ilka
Klinik für Hautkrankheiten - Allgemeine Dermatologie und Venerologie -
Müller, Frank Ulrich
Institut für Pharmakologie und Toxikologie
Schmitz, Martina
Institut für Anatomie und Vaskuläre Biologie
Schmitz, Wilhelm
Institut für Pharmakologie und Toxikologie