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Effects of novel anti-inflammatory compounds on healing of acetic acid-induced gastric ulcer in rats.

机译:新型抗炎化合物对乙酸诱导的大鼠胃溃疡愈合的影响。

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摘要

Nonsteroidal anti-inflammatory drugs often cause development of significant GI lesions. Selective inhibitors of prostaglandin G/H synthase/cyclooxygenase-2 (PGHS-2) enzyme and some dual inhibitors of PGHS/5-lipoxygenase (5-LO) enzymes have been reported to be potent anti-inflammatory compounds that carry a much lower risk of having GI irritating effects. We have evaluated the anti-inflammatory effect and the GI safety profile of three new anti-inflammatory compounds: the selective PGHS-2 inhibitors NS-398 and PD 138387 and the PGHS/5-LO dual inhibitor PD 137968. All the compounds tested showed an anti-inflammatory activity in the carragenan footpad edema test in rats. None of these compounds caused either gastric damage 4 h after p.o. administration of 100 mg/kg in rats or inhibition of PGE2 synthesis in the stomach. However, when administered p.o. at an effective anti-inflammatory dose to rats with pre-existing acetic acid-induced gastric ulcer, NS-398 caused a statistically significant delay of ulcer healing. No impairment of the ulcer healing was observed with the other compounds evaluated. Derivatives of 2,6-di-tert-butylphenol, whose members may act as PGHS-1/PGHS-2 inhibitors, selective PGHS-2 inhibitors or PGHS/5-LO dual inhibitors, are novel anti-inflammatory compounds that are devoid of GI irritating effects and do not affect the rate of pre-existing gastric ulcer healing.
机译:非甾体类抗炎药通常会导致明显的胃肠道病变。据报道,前列腺素G / H合酶/环加氧酶2(PGHS-2)酶的选择性抑制剂和PGHS / 5-脂加氧酶(5-LO)酶的某些双重抑制剂是有效的消炎化合物,其风险要低得多具有胃肠道刺激作用。我们已经评估了三种新型抗炎化合物的抗炎作用和胃肠道安全性:选择性PGHS-2抑制剂NS-398和PD 138387和PGHS / 5-LO双重抑制剂PD137968。所有测试的化合物均显示在大鼠角叉菜胶脚垫浮肿试验中具有抗炎活性。这些化合物均未在p.o后4小时引起胃损害。在大鼠中施用100 mg / kg或抑制胃中PGE2的合成。但是,口服时以有效的抗炎剂量对已存在乙酸诱发的胃溃疡的大鼠,NS-398在统计学上显着延迟了溃疡的愈合。用所评价的其他化合物未观察到溃疡愈合的损害。 2,6-二叔丁基苯酚的衍生物是新型的消炎化合物,其衍生物可作为PGHS-1 / PGHS-2抑制剂,选择性PGHS-2抑制剂或PGHS / 5-LO双重抑制剂。胃肠道刺激性作用且不影响先前存在的胃溃疡愈合的速度。

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