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恩前列素低剂量维持治疗与雷尼替丁预防十二指肠溃疡复发的比较。

A comparison of low-dose maintenance treatment with enprostil against ranitidine in the prevention of duodenal ulcer recurrence.

作者信息

Bardhan K D, Morris P, Hinchliffe R F, Saunders J H, MacDougall B R, Bold J M, Freeman P R

机构信息

District General Hospital, Rotherham, UK.

出版信息

Aliment Pharmacol Ther. 1989 Oct;3(5):489-97. doi: 10.1111/j.1365-2036.1989.tb00240.x.

Abstract

Enprostil, a prostaglandin E2 analogue, is effective in healing acute duodenal ulcer but its value in preventing recurrence, when given daily for maintenance therapy, is uncertain. In this three-centre study we compared enprostil and ranitidine maintenance therapy; the latter is known to reduce duodenal ulcer relapse rates. Patients whose duodenal ulcers had been healed by treatment with an H2-receptor antagonist were randomized to receive single-blind treatment with either 35 micrograms enprostil (n = 64) or 150 mg ranitidine (n = 64) at bedtime for periods of up to 1 year. Endoscopy was routinely performed at 3 months at one centre, and at 6 and 12 months at all three centres, or whenever ulcer symptoms recurred. Clinical assessment and laboratory investigations were performed every 3 months. Relapse, defined as recurrent ulcer with or without pain, or erosions with pain, was significantly greater in patients on enprostil, the comparative rates at 3, 6 and 12 months were: enprostil 23, 31 and 36% ranitidine 6, 12 and 17% (P = 0.013; P = 0.03 and P = 0.03, respectively). Thirty-one patients reported adverse events, the most common being headache (enprostil = 6, ranitidine = 2) and mild diarrhoea (enprostil = 6, ranitidine = 0). Four patients on enprostil were withdrawn for adverse events, although none terminated because of diarrhoea. There were no clinically significant changes in haematology or biochemistry. Enprostil may reduce duodenal ulcer relapse but at a dose of 35 micrograms nightly, it is less effective than 150 mg ranitidine nightly.

摘要

恩前列素是一种前列腺素E2类似物,对急性十二指肠溃疡的愈合有效,但每日用于维持治疗时预防复发的价值尚不确定。在这项三中心研究中,我们比较了恩前列素和雷尼替丁的维持治疗;已知后者可降低十二指肠溃疡复发率。十二指肠溃疡经H2受体拮抗剂治疗愈合的患者被随机分为单盲治疗组,睡前分别服用35微克恩前列素(n = 64)或150毫克雷尼替丁(n = 64),治疗期最长为1年。在一个中心,3个月时常规进行内镜检查,在所有三个中心,6个月和12个月时常规进行内镜检查,或在溃疡症状复发时进行内镜检查。每3个月进行一次临床评估和实验室检查。复发定义为有或无疼痛的复发性溃疡,或有疼痛的糜烂,服用恩前列素的患者复发率显著更高,3个月、6个月和12个月时的比较复发率分别为:恩前列素23%、31%和36%,雷尼替丁6%、12%和17%(P = 0.013;P = 0.03和P = 0.03)。31名患者报告了不良事件,最常见的是头痛(恩前列素 = 6例,雷尼替丁 = 2例)和轻度腹泻(恩前列素 = 6例,雷尼替丁 = 0例)。4例服用恩前列素的患者因不良事件退出研究,尽管没有患者因腹泻而终止治疗。血液学或生物化学方面没有临床上显著的变化。恩前列素可能会降低十二指肠溃疡复发率,但每晚服用35微克时,其效果不如每晚服用150毫克雷尼替丁。

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