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Gastric anti-ulcerative and anti-inflammatory activity of metyrosine in rats.

机译:甲硫氨酸对大鼠胃的抗溃疡和抗炎活性。

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In this study, the anti-inflammatory and anti-ulcerative effects of metyrosine, a selective tyrosine hydroxylase enzyme inhibitor, were investigated in rats. For ulcer experiments, indomethacin-induced gastric ulcer tests and ethanol-induced gastric ulcer tests were used. For these experiments, rats were fasted for 24 h. Different doses of metyrosine and 25 mg/kg doses of ranitidine were administered to rats, followed by indomethacin at 25 mg/kg for the indomethacin-induced ulcer test, or 50% ethanol for the ethanolinduced test. Results have shown that at all of the doses used (50, 100 and 200 mg/kg), metyrosine had significant anti-ulcerative effects in both indomethacin and ethanol-induced ulcer tests. Metyrosine doses of 100 and 200 mg/kg (especially the 200 mg/kg dose) also inhibited carrageenan-induced paw inflammation even more effectively than indomethacin. In addition, to characterize the anti-inflammatory mechanism of metyrosine we investigated its effects on cyclooxygenase (COX) activity in inflammatory tissue (rat paw). The results showed that all doses of metyrosine significantly inhibited high COX-2 activity. The degree of COX-2 inhibition correlated with the increase in anti-inflammatory activity. In conclusion, we found that metyrosine has more anti-inflammatory effects than indomethacin and that these effects can be attributed to the selective inhibition of COX-2 enzymes by metyrosine. We also found that adrenalin levels are reduced upon metyrosine treatment, which may be the cause of the observed gastro-protective effects of this compound
机译:在这项研究中,对甲硫氨酸(一种选择性酪氨酸羟化酶抑制剂)的抗炎和抗溃疡作用进行了研究。对于溃疡实验,使用了消炎痛诱导的胃溃疡试验和乙醇诱导的胃溃疡试验。对于这些实验,大鼠禁食24小时。给大鼠施用不同剂量的甲硫氨酸和25 mg / kg剂量的雷尼替丁,然后用25 mg / kg的吲哚美辛进行吲哚美辛诱导的溃疡试验,或用50%的乙醇进行乙醇诱导试验。结果表明,在使用的所有剂量(50、100和200 mg / kg)下,甲硫氨酸在消炎痛和乙醇诱导的溃疡试验中均具有显着的抗溃疡作用。甲硫氨酸剂量分别为100和200 mg / kg(特别是200 mg / kg剂量),也比消炎痛更有效地抑制了角叉菜胶诱导的足爪炎症。另外,为了表征甲硫氨酸的抗炎机制,我们研究了其对炎性组织(鼠爪)中环氧合酶(COX)活性的影响。结果表明,所有剂量的甲硫氨酸均显着抑制高COX-2活性。 COX-2抑制的程度与抗炎活性的增加相关。总之,我们发现甲硫氨酸比消炎痛具有更强的抗炎作用,并且这些作用可以归因于甲硫氨酸对COX-2酶的选择性抑制。我们还发现,甲硫氨酸治疗后肾上腺素水平降低,这可能是该化合物观察到的胃保护作用的原因

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