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SU-840是一种新型的槐定碱合成黄酮类衍生物,具有强大的胃保护和溃疡愈合活性。

SU-840, a novel synthetic flavonoid derivative of sophoradin, with potent gastroprotective and ulcer healing activity.

作者信息

Brzozowski T, Konturek S J, Kwiecien S, Pajdo R, Drozdowicz D, Sliwowski Z, Muramatsu M

机构信息

Department of Physiology, Jagiellonian University School of Medicine, Cracow, Poland.

出版信息

J Physiol Pharmacol. 1998 Mar;49(1):83-98.

PMID:9594413
Abstract

Flavonois derived from sophoradine are known to exhibit gastroprotective and ulcer healing properties but the mechanism of these actions are not fully explained. In this study we determined the effect of novel flavonoid derivative of sophoradin, SU-840, on gastric secretion, acute gastric lesions induced by acid-independent (100% ethanol) or acid-dependent ulcerogens (acidified aspirin (ASA) and stress) and on the healing of chronic gastric ulcers in rats. The number and area of gastric lesions was determined by planimetry, gastric blood flow (GBF) was measured using H2-gas clearance technique and the mucosal samples were excised for the measurement of PGE2 generation by radioimmunoassay. Exposure of rats to 100% ethanol or acidified ASA (100 mg/kg dissolved in 0.2 N HCl) or to water immersion and restraint stress (WRS) resulted in hemorrhagic gastric lesions accompanied by drastic fall in the GBF as compared to the values recorded in vehicle treated gastric mucosa. SU-840 (6.25-100 mg/kg i.g.) reduced dose-dependently gastric acid and pepsin secretion and gastric lesions induced by ethanol, acidified ASA and WRS, the dose inhibiting by 50% of these lesions (ID50) being 28, 17 and 95 mg/kg, respectively. This protection required much lower doses as compared to original sofalcone or sucralfate and was obtained when this sofalcone-like drug was administered via parenteral route. The protective effect of SU-840 given i.g. or i.p. was accompanied by a marked rise in the GBF and mucosal generation of PGE2. The protective activity of SU-840 showed longer duration of the action than that of sofalcone and occurred in the doses that failed to affect gastric secretion. Pretreatment with indomethacin to suppress endogenous PG reversed completely the protective and hyperemic effects of SU-840 against ethanol and stress induced damage whereas L-NNA, a potent inhibitor of NO-synthase, failed to affect protection but completely abolished the hyperemia evoked by this agent. NEM, an sulfhydryl alkylator, significantly attenuated the protective and hyperemic effects of SU-840 suggesting that endogenous sulfhydryls are involved in these effects. Seven day treatment with SU-840 accelerated significantly healing rate of chronic gastric ulcers and increased the GBF at the ulcer crater and ulcer margin. These effects were reversed by L-NNA and further restored by the addition to L-NNA of L-arginine, a substrate for NO-synthase. We conclude that SU-840 exhibits gastroprotective and hyperemic activity against acid-independent and acid-dependent irritants involving endogenous PG, sulfhydryls and hyperemia mediated by NO and 2) enhancement in gastric blood flow in the ulcer area mediated by NO appears to be essential for the acceleration of the ulcer healing by SU-840.

摘要

已知从槐定碱衍生而来的黄酮类化合物具有胃保护和促进溃疡愈合的特性,但其作用机制尚未完全阐明。在本研究中,我们测定了槐定碱新型黄酮类衍生物SU - 840对胃分泌、由非酸依赖性(100%乙醇)或酸依赖性致溃疡剂(酸化阿司匹林(ASA)和应激)诱导的急性胃损伤以及对大鼠慢性胃溃疡愈合的影响。通过平面测量法确定胃损伤的数量和面积,使用氢气清除技术测量胃血流量(GBF),并切除黏膜样本通过放射免疫测定法测量PGE2的生成。与给予赋形剂处理的胃黏膜所记录的值相比,将大鼠暴露于100%乙醇或酸化ASA(100 mg/kg溶于0.2 N HCl)或水浸束缚应激(WRS)会导致出血性胃损伤,并伴有GBF的急剧下降。SU - 840(6.25 - 100 mg/kg,腹腔注射)剂量依赖性地减少胃酸和胃蛋白酶分泌以及由乙醇、酸化ASA和WRS诱导的胃损伤,抑制这些损伤50%的剂量(ID50)分别为28、17和95 mg/kg。与原索法酮或硫糖铝相比,这种保护所需剂量要低得多,并且当这种类索法酮药物通过非肠道途径给药时即可获得。经口或腹腔注射给予SU - 840的保护作用伴随着GBF的显著升高和黏膜PGE2的生成。SU - 840的保护活性显示出比索法酮更长的作用持续时间,并且在不影响胃分泌的剂量下即可出现。用吲哚美辛预处理以抑制内源性PG可完全逆转SU - 840对乙醇和应激诱导损伤的保护和充血作用,而L - NNA(一种有效的一氧化氮合酶抑制剂)未能影响保护作用,但完全消除了该药物引起的充血。NEM(一种巯基烷化剂)显著减弱了SU - 840的保护和充血作用,表明内源性巯基参与了这些作用。用SU - 840进行为期7天的治疗可显著加速慢性胃溃疡的愈合速度,并增加溃疡 crater 和溃疡边缘的GBF。这些作用被L - NNA逆转,并通过向L - NNA中添加L - 精氨酸(一氧化氮合酶的底物)进一步恢复。我们得出结论:1)SU - 840对非酸依赖性和酸依赖性刺激物表现出胃保护和充血活性,涉及内源性PG、巯基以及由NO介导的充血;2)由NO介导的溃疡区域胃血流量增加似乎是SU - 840加速溃疡愈合所必需的。

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