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昂丹司琼与慢性肝病瘙痒:一项对照研究。

Ondansetron and pruritus in chronic liver disease: a controlled study.

作者信息

Jones E Anthony, Molenaar Hugo A J, Oosting Johannes

机构信息

Department of Gastrointestinal and Liver Diseases, Academic Medical Center, Amsterdam, Netherlands.

出版信息

Hepatogastroenterology. 2007 Jun;54(76):1196-9.

Abstract

BACKGROUND/AIMS: Increased central opioidergic neurotransmission, mediated by endogenous opioid peptide agonists, contributes to the pruritus of cholestasis. There are interrelationships between the opioid and serotonin neurotransmitter systems. The serotonin 5-HT3 receptor subtype antagonist, ondansetron, has been reported to ameliorate centrally-mediated pruritus induced by exogenously administered opiates. This study was designed to determine whether long-term oral administration of ondansetron is efficacious in ameliorating pruritus complicating chronic liver disease.

METHODOLOGY

Seventeen patients with severe pruritus complicating established chronic liver disease were randomized to receive, double-blind, ondansetron (8 mg) or a placebo orally; each was administered thrice daily for a 4-week period. Endpoints were subjective scores of pruritus and objective 24-hour measurements of scratching activity. Analysable data were generated in 13 of the patients.

RESULTS

Ondansetron therapy was associated with ameliorations of pruritus that appeared to be clinically significant in 5 patients (38%); in these 5 patients the mean decrease in a subjective score of pruritus was 27% of the scale of the score. However, these apparent ameliorations were not associated with robust decreases in scratching activity. For the whole group of 13 patients mean scratching activity during ondansetron therapy was not significantly less than that during treatment with placebo (p = 0.19). The total time that patients were not scratching was similar during treatment with ondansetron and placebo (p = 0.57).

CONCLUSIONS

The findings suggest that serotoninergic neurotransmission, in neurons bearing receptors of the 5-HT3 subtype, plays no more than a minor role in the mediation of pruritus complicating chronic liver disease. The lack of an association between the results of applying subjective scores of pruritus and scratching activity emphasizes the need to include an objective quantitative efficacy endpoint in the design of trials of new therapies for pruritus.

摘要

背景/目的:由内源性阿片肽激动剂介导的中枢阿片能神经传递增加,会导致胆汁淤积性瘙痒。阿片和5-羟色胺神经递质系统之间存在相互关系。据报道,5-羟色胺5-HT3受体亚型拮抗剂昂丹司琼可改善外源性给予阿片类药物引起的中枢介导性瘙痒。本研究旨在确定长期口服昂丹司琼是否能有效改善慢性肝病并发的瘙痒。

方法

17例患有严重瘙痒且已确诊为慢性肝病的患者被随机分为两组,进行双盲试验,一组口服昂丹司琼(8毫克),另一组口服安慰剂;每组每日给药3次,持续4周。观察终点为瘙痒的主观评分和抓挠活动的客观每日测量值。13例患者产生了可分析的数据。

结果

昂丹司琼治疗与瘙痒改善相关,5例患者(38%)的改善似乎具有临床意义;在这5例患者中,瘙痒主观评分的平均降低幅度为评分量表的27%。然而,这些明显的改善与抓挠活动的显著减少无关。对于13例患者的整个组,昂丹司琼治疗期间的平均抓挠活动并不显著低于安慰剂治疗期间(p = 0.19)。在昂丹司琼和安慰剂治疗期间,患者无抓挠的总时间相似(p = 0.57)。

结论

这些发现表明,在表达5-HT3亚型受体的神经元中,5-羟色胺能神经传递在慢性肝病并发瘙痒的介导中所起的作用不大。瘙痒主观评分结果与抓挠活动之间缺乏相关性,这强调了在瘙痒新疗法试验设计中纳入客观定量疗效观察终点的必要性。

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