PF-10040对实验性nsaid -胃炎的保护作用:白细胞、白三烯和PAF的作用。

Journal of lipid mediators Pub Date : 1993-06-01
J L Wallace, G W McKnight, D Donigi-Gale, T S Shoupe, D N Granger
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引用次数: 0

摘要

采用非甾体抗炎药-胃炎实验模型研究喹啉衍生物PF-10040的作用及机制。口服PF-10040剂量依赖性地降低了吲哚美辛引起的胃损伤的严重程度,当剂量为10 mg/kg或更大时,观察到显著的保护作用。该化合物的保护作用在给药后持续长达6小时。PF-10040还能显著降低阿司匹林或萘普生引起的胃损伤的严重程度。在保护剂量下,PF-10040对胃LTB4合成、LTB4诱导的粒细胞向皮内注射部位募集或ltd4诱导的胃血流变化没有显著影响。通过体外实验检测了PF-10040对自由基的清除作用,结果表明,在高达10 mM的浓度下,PF-10040对胃酸分泌没有显著影响。在大鼠肠系膜小静脉中,PF-10040抑制PAF-,但不抑制ltb4诱导的白细胞粘附和迁移。这些结果表明,PF-10040的保护作用不是由于清除自由基、抑制白三烯合成、阻断LTB4或LTD4受体或抑制LTB4介导的白细胞内皮细胞粘附。
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Protective effects of PF-10040 in experimental NSAID-gastritis: role of leukocytes, leukotrienes and PAF.

The effects and mechanism of action of PF-10040, a quinoline derivative, were examined in an experimental model of NSAID-gastritis. Oral pretreatment with PF-10040 dose-dependently reduced the severity of indomethacin-induced gastric damage, with a significant protective effect being observed with doses of 10 mg/kg or greater. The protective effects of this compound persisted for as long as 6 h after administration. PF-10040 also significantly reduced the severity of aspirin- or naproxen-induced gastric damage. At protective doses, PF-10040 did not significantly affect gastric LTB4 synthesis, LTB4-induced granulocyte recruitment to intradermal injection sites, or LTD4-induced changes in gastric blood flow. The free radical scavenging effects of PF-10040 were examined using an in vitro assay, in which it failed to exert significant effects at concentrations of up to 10 mM. PF-10040 had no significant effect on gastric acid secretion. In rat mesenteric venules, PF-10040 inhibited PAF-, but not LTB4-induced leukocyte adherence and emigration. These results suggest that the protective effects of PF-10040 are not attributable to scavenging of free radicals, inhibition of leukotriene synthesis, blockade of LTB4 or LTD4 receptors or inhibition of LTB4-mediated leukocyte endothelial cell adhesion.

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