Abstract:The aim of the present study was to assess the acute motility effects and desensitizing activity of the stable ATP analogue and P 2X purinoceptor agonist a,b-methylene ATP (a,b-meATP) and the effect of a,b-meATP desensitization on nerve-mediated cholinergic responses in the guinea-pig ileum in vitro. It was confirmed that a,b-meATP (1-30 mM) causes neurally-mediated, cholinergic (tetrodotoxin-and atropine-sensitive) longitudinal contractions. These responses were not influenced by the ganglionic blocking drug hexamethonium (50 mM), or a combination of the adrenergic neurone blocking drug guanethidine (3 mM), the opioid receptor antagonist naloxone (0.5 mM) and the nitric oxide synthase inhibitor N Gnitro-L-arginine (L-NOARG; 100 mM), but were strongly reduced or abolished by the P 2 purinoceptor antagonist PPADS (30 mM) or by tachyphylaxis evoked by 10 mM a,b-meATP. The contractile effect of a,b-meATP (3 mM) was moderately inhibited by 10 mM and strongly suppressed by 30 mM of NF 279, an antagonist predominantly affecting P2X 1 purinoceptors, but left uninfluenced by the P2X 5,7 receptor antagonist Brilliant blue G. No relaxant effect of a,b-meATP was detected in the concentration range of 1-30 mM. Tachyphylaxis to a,b-meATP (1-10 mM) caused a moderate inhibition of the cholinergic (atropine-sensitive) contractile response of the ileum to electrical field stimulation (5 Hz for 5 sec.). This reduction was unaltered in the presence of guanethidine, naloxone and L-NOARG. Responses to nicotine (1 or 2 mM) were not reduced by a,b-meATP tachyphylaxis. It is suggested that a,b-meATP-sensitive P 2X purinoceptors are involved in the prejunctional modulation of cholinergic neurotransmission between the myenteric plexus and longitudinal smooth muscle in the guinea-pig small intestine.a,b-Methylene ATP (a,b-meATP) is an analogue of adenosine-5'-triphoshate (ATP) with a greater metabolic stability than the parent compound. Though its spectrum of agonist activity at various purinoceptors is somewhat different from that of ATP itself (Lambrecht 2000 for review) a,b-meATP is one of the traditional drugs used for studying purinergic mechanisms (Ralevic & Burnstock 1998;Lambrecht 2000). In addition to stimulating some subtypes of P 2X purinoceptors, a,b-meATP can induce powerful tachyphylaxis on these receptors, which has been exploited in the identification of endogenous ATP as neurotransmitter, e.g. in the urinary bladder (Ralevic & Burnstock 1998).Our recent work indicated that the P 2 purinoceptor antagonist PPADS and suramin, two P 2 purinoceptor antagonists of limited subtype selectivity reduced cholinergic longitudinal contractions of the guinea-pig small intestine in vitro (Barthó et al. 1997). Several lines of evidence suggest that this effect reflect an involvement of PPADS-and suramin-sensitive P 2 purinoceptors in the mediation/positive modulation of cholinergic contractions, rather than a nonspecific action (Barthó et al. 1997). In the present work we attempt to approach this problem with a,b-meATP tachyphyl...
