AUTHOR=Mosshammer Anna , Zou Lifang , Boehm Stefan , Schicker Klaus 

TITLE=Mechanisms of sympathoexcitation via P2Y6 receptors

JOURNAL=Frontiers in Pharmacology

VOLUME=13

YEAR=2022

URL=https://www.frontiersin.org/journals/pharmacology/articles/10.3389/fphar.2022.1014284

DOI=10.3389/fphar.2022.1014284

ISSN=1663-9812

ABSTRACT=<p>Many drugs used in cardiovascular therapy, such as angiotensin receptor antagonists and beta-blockers, may exert at least some of their actions through effects on the sympathetic nervous system, and this also holds true for e.g., P2Y<sub>12</sub> antagonists. A new target at the horizon of cardiovascular drugs is the P2Y<sub>6</sub> receptor which contributes to the development of arteriosclerosis and hypertension. To learn whether P2Y<sub>6</sub> receptors in the sympathetic nervous system might contribute to actions of respective receptor ligands, responses of sympathetic neurons to P2Y<sub>6</sub> receptor activation were analyzed in primary cell culture. UDP in a concentration dependent manner caused membrane depolarization and enhanced numbers of action potentials fired in response to current injections. The excitatory action was antagonized by the P2Y<sub>6</sub> receptor antagonist MRS2578, but not by the P2Y<sub>2</sub> antagonist AR-C118925XX. UDP raised intracellular Ca<sup>2+</sup> in the same range of concentrations as it enhanced excitability and elicited inward currents under conditions that favor Cl<sup>−</sup> conductances, and these were reduced by a blocker of Ca<sup>2+</sup>-activated Cl<sup>−</sup> channels, CaCCInh-A01. In addition, UDP inhibited currents through K<sub>V</sub>7 channels. The increase in numbers of action potentials caused by UDP was not altered by the K<sub>V</sub>7 channel blocker linopirdine, but was enhanced in low extracellular Cl<sup>−</sup> and was reduced by CaCCInh-A01 and by an inhibitor of phospholipase C. Moreover, UDP enhanced release of previously incorporated [3H] noradrenaline, and this was augmented in low extracellular Cl<sup>−</sup> and by linopirdine, but attenuated by CaCCInh-A01. Together, these results reveal sympathoexcitatory actions of P2Y<sub>6</sub> receptor activation involving Ca<sup>2+</sup>-activated Cl<sup>−</sup> channels.</p>