Specific inhibition of the transporter MRP4/ABCC4 affects multiple signaling pathways and thrombus formation in human platelets
Robert Wolf,
Sophie Grammbauer,
Raghavendra Palankar,
Céline Tolksdorf,
Eileen Moritz,
Andreas Böhm,
Mahmoud Hasan,
Annika Hafkemeyer,
Andreas Greinacher,
Mladen V. Tzvetkov,
Bernhard H. Rauch,
Gabriele Jedlitschky
Affiliations
Robert Wolf
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald, Germany; German Center for Cardiovascular Research (DZHK), Partner Site Greifswald
Sophie Grammbauer
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald
Raghavendra Palankar
Department of Immunology and Transfusion Medicine, University Medicine Greifswald, Greifswald
Céline Tolksdorf
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald, Germany; Department of Human Medicine, Section of Pharmacology and Toxicology, Carl von Ossietzky University of Oldenburg, Oldenburg
Eileen Moritz
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald, Germany; German Center for Cardiovascular Research (DZHK), Partner Site Greifswald
Andreas Böhm
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald
Mahmoud Hasan
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald
Annika Hafkemeyer
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald
Andreas Greinacher
Department of Immunology and Transfusion Medicine, University Medicine Greifswald, Greifswald
Mladen V. Tzvetkov
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald
Bernhard H. Rauch
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald, Germany; German Center for Cardiovascular Research (DZHK), Partner Site Greifswald, Germany; Department of Human Medicine, Section of Pharmacology and Toxicology, Carl von Ossietzky University of Oldenburg, Oldenburg
Gabriele Jedlitschky
Department of General Pharmacology, Center of Drug Absorption and Transport (C_DAT), Greifswald
The multidrug resistance protein 4 (MRP4) is highly expressed in platelets and several lines of evidence point to an impact on platelet function. MRP4 represents a transporter for cyclic nucleotides as well as for certain lipid mediators. The aim of the present study was to comprehensively characterize the effect of a short-time specific pharmacological inhibition of MRP4 on signaling pathways in platelets. Transport assays in isolated membrane vesicles showed a concentrationdependent inhibition of MRP4-mediated transport of cyclic nucleotides, thromboxane (Tx)B2 and fluorescein (FITC)- labeled sphingosine-1-phosphate (S1P) by the selective MRP4 inhibitor Ceefourin-1. In ex vivo aggregometry studies in human platelets, Ceefourin-1 significantly inhibited platelet aggregation by about 30-50% when ADP or collagen was used as activating agents, respectively. Ceefourin-1 significantly lowered the ADP-induced activation of integrin aIIbb3, indicated by binding of FITC-fibrinogen (about 50% reduction at 50 mM Ceefourin-1), and reduced calcium influx. Furthermore, pre-incubation with Ceefourin-1 significantly increased PGE1- and cinaciguat-induced vasodilatorstimulated phosphoprotein (VASP) phosphorylation, indicating increased cytosolic cAMP as well as cGMP concentrations, respectively. The release of TxB2 from activated human platelets was also attenuated. Finally, selective MRP4 inhibition significantly reduced both the total area covered by thrombi and the average thrombus size by about 40% in a flow chamber model. In conclusion, selective MRP4 inhibition causes reduced platelet adhesion and thrombus formation under flow conditions. This finding is mechanistically supported by inhibition of integrin aIIbb3 activation, elevated VASP phosphorylation and reduced calcium influx, based on inhibited cyclic nucleotide and thromboxane transport as well as possible further mechanisms.
