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哌仑西平对十二指肠溃疡患者胰多肽释放的可能作用:一项随机交叉研究的初步结果

Possible role of pirenzepine on the release of pancreatic polypeptide in duodenal ulcer patients: preliminary results of a randomized cross-over study.

作者信息

Gasbarrini G, Tovoli S, Giorgi-Conciato M, Severi D, Bonvicini F, Caletti G

出版信息

Int J Tissue React. 1983;5(4):379-85.

PMID:6689490
Abstract

The effects of repeated oral doses of pirenzepine (100 mg daily for 7 days) and antacid (Maalox, 105 ml daily for 7 days) on the test-meal-stimulated release of pancreatic polypeptide (PP) were evaluated in 7 duodenal ulcer outpatients by means of a randomized cross-over study, with a wash-out period of one week between pirenzepine and antacid administration. The effects of pirenzepine (100 mg daily for 7 days) were also evaluated in 5 healthy adult volunteers. The stimulus test was performed on each fasting patient two days before the treatment started and after a 7-day treatment. Venous blood samples were obtained before the test meal (basal) and 3, 10 and 30 minutes after it. Plasma PP levels were estimated by means of a specific RIA. The results obtained showed that pirenzepine significantly inhibits the PP response to the test meal in the duodenal ulcer patients and in the healthy volunteers. The above-mentioned effects suggest that one of the mechanisms of action on the therapeutic activity of pirenzepine on peptic ulcer might be explained by the preservation of pancreatic secretion unimpaired by an increase in PP release after meal stimulus.

摘要

通过随机交叉研究,在7例十二指肠溃疡门诊患者中评估了重复口服哌仑西平(每日100毫克,共7天)和抗酸剂(氢氧化铝镁,每日105毫升,共7天)对试餐刺激的胰多肽(PP)释放的影响,在哌仑西平和抗酸剂给药之间有一周的洗脱期。还在5名健康成年志愿者中评估了哌仑西平(每日100毫克,共7天)的效果。在治疗开始前两天和7天治疗后,对每位空腹患者进行刺激试验。在试餐(基础)前以及试餐后3、10和30分钟采集静脉血样。通过特定的放射免疫分析法估计血浆PP水平。获得的结果表明,哌仑西平显著抑制十二指肠溃疡患者和健康志愿者对试餐的PP反应。上述作用表明,哌仑西平对消化性溃疡治疗活性的作用机制之一可能是通过在餐后刺激后PP释放增加而保持胰腺分泌不受损害来解释。

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