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钙拮抗剂丙基 - 亚甲二氧基茚的抗溃疡活性——I. 对大鼠冷/束缚应激诱导溃疡的影响

Antiulcer activity of the calcium antagonist propyl-methylenedioxyindene--I. Effect on cold/restraint stress-induced ulcers in rats.

作者信息

Wong W S, Rahwan R G

机构信息

Division of Pharmacology, Ohio State University, Columbus 43210.

出版信息

Gen Pharmacol. 1990;21(3):321-5. doi: 10.1016/0306-3623(90)90831-6.

Abstract
  1. Propyl-methylenedioxyindene (pr-MDI) is an intracellularly acting calcium antagonist with H2-receptor blocking properties. Stimulus-secretion coupling is inhibited by much lower concentrations of pr-MDI than is excitation-contraction coupling. 2. Since the processes leading to gastric ulceration are calcium-dependent, the aim of this study was to determine if pr-MDI could provide useful antiulcer activity at doses below those required to produce cardiovascular effects. 3. The antiulcer activity of pr-MDI (10-30 mg/kg) was examined in the cold (4 degree C)/restraint (3 hr) stress-induced ulcer model in male rats, and compared with the effects of the H2-blocker cimetidine (10-30 mg/kg) and the calcium channel blocker verapamil (11-32 mg/kg). The drugs were administered intraperitoneally 10 min prior to the cold/restraint stress. 4. All three drugs significantly reduced the number of ulcers and the cumulative length of ulcerated stomach surface in a roughly dose-dependent and equivalent manner. However, whereas the antiulcer doses of verapamil were extremely high, those of pr-MDI were one-sixth to one-half of its antiarrhythmic ED50 in rodents.
摘要
  1. 丙基 - 亚甲二氧基茚(pr - MDI)是一种具有H2受体阻断特性的细胞内作用钙拮抗剂。与兴奋 - 收缩偶联相比,pr - MDI抑制刺激 - 分泌偶联所需的浓度要低得多。2. 由于导致胃溃疡形成的过程是钙依赖性的,本研究的目的是确定pr - MDI在低于产生心血管效应所需剂量时是否能提供有用的抗溃疡活性。3. 在雄性大鼠的冷(4℃)/束缚(3小时)应激诱导溃疡模型中检测了pr - MDI(10 - 30毫克/千克)的抗溃疡活性,并与H2阻滞剂西咪替丁(10 - 30毫克/千克)和钙通道阻滞剂维拉帕米(11 - 32毫克/千克)的作用进行了比较。在冷/束缚应激前10分钟腹腔注射药物。4. 所有三种药物均以大致剂量依赖性且等效的方式显著减少溃疡数量和溃疡胃表面的累积长度。然而,维拉帕米的抗溃疡剂量极高,而pr - MDI的抗溃疡剂量是其在啮齿动物中的抗心律失常ED50的六分之一至二分之一。

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