Received for publication April 21, 2008.
Revised June 25, 2008.
Accepted for publication June 25, 2008.

Activation of the A₃ Adenosine Receptor Suppresses Superoxide Production and Chemotaxis of Mouse Bone Marrow Neutrophils

Abstract

Adenosine is formed in injured/ischemic tissues where it suppresses the actions of essentially all cells of the immune system. Most of the anti-inflammatory actions of adenosine have been attributed to signaling through the G_s protein-coupled A_2A adenosine receptor (AR). Here, we report that the A₃AR is highly expressed in murine neutrophils isolated from bone marrow. Selective activation of the A₃AR with CP-532,903 potently inhibited mouse bone marrow neutrophil superoxide generation and chemotaxis induced by various activating agents. The selectivity of CP-532,903 was confirmed in assays using neutrophils obtained from A_2AAR and A₃AR gene "knock-out" mice. In a model of thioglycollate-induced inflammation, treating mice with CP-532,903 inhibited recruitment of leukocytes into the peritoneum by specifically activating the A₃AR. Collectively, our findings support the theory that the A₃AR contributes to the anti-inflammatory actions of adenosine on neutrophils, and provide a potential mechanistic explanation for the efficacy of A₃AR agonists in animal models of inflammation, i.e., inhibition of neutrophil-mediated tissue injury.

Key words: Adenosine, Leukocytes/Mast cells

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