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Aggressiveness, hypoalgesia and high blood pressure in mice lacking the adenosine A2a receptor
被引:0
|作者:
Catherine Ledent
Jean-Marie Vaugeois
Serge N. Schiffmann
Thierry Pedrazzini
Malika El Yacoubi
Jean-Jacques Vanderhaeghen
Jean Costentin
John K. Heath
Gilbert Vassart
Marc Parmentier
机构:
[1] IRIBHN,Division of Hypertension
[2] Université Libre de Bruxelles,Department of Biochemistry
[3] Campus Erasme,undefined
[4] Laboratoire de Recherche sur les Neuropeptides,undefined
[5] Université Libre de Bruxelles,undefined
[6] Campus Erasme,undefined
[7] Service de Génétique Médicale,undefined
[8] Université Libre de Bruxelles,undefined
[9] Campus Erasme,undefined
[10] IFRMP,undefined
[11] Unité de Neuropsychopharmacologie Expérimentale,undefined
[12] CNRS UPRESA 6036,undefined
[13] Faculté de Médecine et de Pharmacie,undefined
[14] Avenue de l'Université,undefined
[15] Lausanne University Medical School,undefined
[16] CRC Growth Factors,undefined
[17] University of Oxford,undefined
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摘要:
Adenosine is released from metabolically active cells by facilitated diffusion, and is generated extracellularly by degradation of released ATP. It is a potent biological mediator that modulates the activity of numerous cell types, including various neuronal populations, platelets, neutrophils and mast cells, and smooth muscle cells in bronchi and vasculature. Most of these effects help to protect cells and tissues during stress conditions such as ischaemia. Adenosine mediates its effects through four receptor subtypes: the A1, A2a, A2b and A3 receptors1. The A2a receptor (A2aR)2,3 is abundant in basal ganglia, vasculature and platelets, and stimulates adenylyl cyclase. It is a major target of caffeine, the most widely used psychoactive drug4. Here we investigate the role of the A2a receptor by disrupting the gene in mice. We found that A2aR-knockout (A2aR−/−) mice were viable and bred normally. Their exploratory activity was reduced, whereas caffeine, which normally stimulates exploratory behaviour, became a depressant of exploratory activity. Knockout animals scored higher in anxiety tests, and male mice were much more aggressive towards intruders. The response of A2aR−/−mice to acute pain stimuli was slower. Blood pressure and heart rate were increased, as well as platelet aggregation. The specific A2a agonist CGS 21680 lost its biological activity in all systems tested.
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页码:674 / 678
页数:4
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