Mulè Flavia, Amato Antonella, Baldassano Sara, Serio Rosa
Dipartimento di Biologia cellulare e dello Sviluppo, Università di Palermo, 90128 Palermo, Italia.
Pharmacol Res. 2007 Aug;56(2):132-9. doi: 10.1016/j.phrs.2007.04.019. Epub 2007 May 10.
It is well accepted that endogenous cannabinoids and CB1 receptors are involved in the regulation of smooth muscle contractility and intestinal motility, through a mechanism mainly related to reduction of acetylcholine release from cholinergic nerve endings. Because, few data exist on a possible modulatory action of the cannabinoid agents on the non-adrenergic non-cholinergic (NANC) excitatory and inhibitory neurotransmission, the aim of the present study was to investigate the effects of cannabinoid drugs on the NANC responses elicited by electrical field stimulation (EFS) in the circular muscle of mouse proximal colon. Colonic contractions were monitored as changes in endoluminal pressure. In NANC conditions, EFS evoked TTX-sensitive responses, characterized by a relaxation, nitrergic in origin, followed by a contraction. The EFS-evoked contraction was significantly reduced by SR48968, NK2 receptor antagonist, and abolished by co-administration of SR48968 and SR140333, NK1 receptor antagonist, suggesting that it was due to release of tachykinins. The cannabinoid receptor synthetic agonist, WIN55,212-2, the putative endogenous ligand, anandamide, the selective CB1 receptor agonist ACEA, but not the selective CB2 receptor agonist JWH-015, produced a concentration-dependent reduction of the NANC contractile responses, without affecting the NANC relaxation. ACEA or anandamide did not modify the contractions induced by exogenous [beta-Ala(8)]-NKA(4-10), agonist of NK2 receptors. The selective antagonist of CB1 receptors, SR141716A, per se failed to affect the EFS-evoked responses, but antagonized the inhibitory effects of WIN55,212-2, anandamide and ACEA on NANC contractile responses. AM630, CB2 receptor antagonist, did not modify the inhibitory effects of WIN55,212-2 or anandamide. URB597, inhibitor of the fatty acid amide hydrolase, enzyme which catalyze the hydrolysis of anandamide, was without any effect on the NANC evoked responses. We conclude that the activation of prejunctional CB1 receptors produces inhibition of NANC contractile responses in mouse colonic preparations. However, endogenous ligands do not seem to modulate tonically the NANC transmission in mouse colon.
内源性大麻素和CB1受体通过一种主要与减少胆碱能神经末梢乙酰胆碱释放相关的机制参与平滑肌收缩性和肠道运动的调节,这一点已被广泛接受。由于关于大麻素类药物对非肾上腺素能非胆碱能(NANC)兴奋性和抑制性神经传递可能的调节作用的数据很少,本研究的目的是研究大麻素药物对电场刺激(EFS)在小鼠近端结肠环行肌中引发的NANC反应的影响。结肠收缩通过腔内压力变化进行监测。在NANC条件下,EFS诱发对河豚毒素敏感的反应,其特征是起源于一氧化氮能的舒张,随后是收缩。EFS诱发的收缩被NK2受体拮抗剂SR48968显著降低,并被SR48968和NK1受体拮抗剂SR140333共同给药所消除,这表明它是由于速激肽的释放。大麻素受体合成激动剂WIN55,212-2、假定的内源性配体花生四烯酸乙醇胺、选择性CB1受体激动剂ACEA,但不是选择性CB2受体激动剂JWH-015,产生了浓度依赖性的NANC收缩反应降低,而不影响NANC舒张。ACEA或花生四烯酸乙醇胺没有改变由NK2受体激动剂外源性[β-丙氨酸(8)]-神经激肽A(4-10)诱导的收缩。CB1受体的选择性拮抗剂SR141716A本身未能影响EFS诱发的反应,但拮抗了WIN55,212-2、花生四烯酸乙醇胺和ACEA对NANC收缩反应的抑制作用。CB2受体拮抗剂AM630没有改变WIN55,212-2或花生四烯酸乙醇胺的抑制作用。脂肪酸酰胺水解酶(催化花生四烯酸乙醇胺水解的酶)抑制剂URB597对NANC诱发的反应没有任何影响。我们得出结论,在小鼠结肠制剂中,节前CB1受体的激活会抑制NANC收缩反应。然而,内源性配体似乎不会对小鼠结肠中的NANC传递进行紧张性调节。
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