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吲哚美辛和萘丁美酮对大鼠前列腺素介导的胃对中枢迷走神经激活反应的不同影响。

Different effects of indomethacin and nabumetone on prostaglandin-mediated gastric responses to central vagal activation in rats.

作者信息

Cardin S, Soll A H, Taché Y

机构信息

CURE/Digestive Disease Center, West Los Angeles VA Medical Center, California, USA.

出版信息

J Pharmacol Exp Ther. 1995 Nov;275(2):667-73.

PMID:7473153
Abstract

Intracisternal injection of a stable thyrotropin-releasing hormone (TRH) analog increases gastric prostaglandins release and mucosal resistance to injury through central vagal pathways. The effects of two nonsteroidal anti-inflammatory drugs, indomethacin (INDO) and nabumetone on intracisternal injection of various doses of TRH-induced gastric acid secretion and changes in mucosal resistance were investigated in urethane-anesthetized rats. Doses of INDO (5 mg/kg) and nabumetone (13.75 mg/kg) producing similar acute anti-inflammatory response in the carrageenin-induced paw edema were injected i.p. in all studies. INDO potentiated the acid secretion induced by intracisternal injection of TRH at 25, 50 and 200 ng by 5.1-, 1.9- and 1.4-fold, respectively, whereas nabumetone did not modify the secretory response to TRH. Moderate erosions were observed in 100% of rats treated with the combination of INDO and TRH (200 ng) whereas no erosions were observed when TRH or INDO were given alone or TRH in combination with nabumetone. TRH at 7 ng reduced mucosal damage induced by intragastric administration of ethanol (60%, 1 ml/kg) by 63%. The mucosal protective action of TRH was abolished by INDO but not altered by nabumetone pretreatment. These data indicate that at comparable anti-inflammatory doses, nabumetone, unlike INDO, neither blocks the protection against ethanol injury induced by low doses of TRH injected intracisternally nor potentiates the gastric acid secretion or lesions induced by higher dose of TRH. We speculate that these differences reflect reduced inhibition of gastric prostaglandins by nabumetone.

摘要

脑池内注射一种稳定的促甲状腺激素释放激素(TRH)类似物可通过中枢迷走神经途径增加胃前列腺素的释放以及黏膜对损伤的抵抗力。在氨基甲酸乙酯麻醉的大鼠中,研究了两种非甾体抗炎药吲哚美辛(INDO)和萘丁美酮对脑池内注射不同剂量TRH诱导的胃酸分泌及黏膜抵抗力变化的影响。在所有研究中,腹腔注射产生类似角叉菜胶诱导爪肿胀急性抗炎反应的INDO剂量(5 mg/kg)和萘丁美酮剂量(13.75 mg/kg)。INDO分别使脑池内注射25、50和200 ng TRH诱导的胃酸分泌增强5.1倍、1.9倍和1.4倍,而萘丁美酮未改变对TRH的分泌反应。100%接受INDO与TRH(200 ng)联合治疗的大鼠出现中度糜烂,而单独给予TRH或INDO或TRH与萘丁美酮联合给药时未观察到糜烂。7 ng的TRH使胃内给予乙醇(60%,1 ml/kg)诱导的黏膜损伤减少63%。TRH的黏膜保护作用被INDO消除,但未被萘丁美酮预处理改变。这些数据表明,在相当的抗炎剂量下,与INDO不同,萘丁美酮既不阻断脑池内注射低剂量TRH诱导的对乙醇损伤的保护作用,也不增强高剂量TRH诱导的胃酸分泌或损伤。我们推测这些差异反映了萘丁美酮对胃前列腺素的抑制作用减弱。

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