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肝硬化患者终生酒精摄入量的测量:可重复性及临床相关性

The measure of life-time alcohol consumption in patients with cirrhosis: reproducibility and clinical relevance.

作者信息

Arico S, Galatola G, Tabone M, Corrao G, Torchio P, Valenti M, De la Pierre M

机构信息

Division of Gastroenterology, Ospedale Mauriziano Umberto I, Torino, Italy.

出版信息

Liver. 1995 Aug;15(4):202-8. doi: 10.1111/j.1600-0676.1995.tb00671.x.

Abstract

Our aims were to design a reproducible method of measuring life-time alcohol consumption in patients with cirrhosis, and to assess the risk of liver decompensation associated with alcohol intake using a case-control design and a multivariate analysis. We studied 439 patients ("cases") with decompensated cirrhosis, and 233 with compensated cirrhosis ("controls"). Mean life-time daily amount and duration of alcohol intake were measured by a standardized questionnaire, whose reproducibility, assessed by interviewing 75 relatives, was 70% for daily alcohol intake and 84% for duration of intake. Better reproducibility was found by re-interviewing patients at discharge from hospital. Daily alcohol intake was significantly higher in males, younger patients and patients with liver decompensation. After stratification according to the average life-time daily alcohol intake, we found a significant increase in the risk of liver decompensation from 125 g ethanol intake per day onwards. No association was found between duration of alcohol intake and risk of liver decompensation. We conclude that alcohol intake can be reliably and reproducibly measured: in patients with cirrhosis, increased alcohol intake is associated with increased risk of liver decompensation, with a significant dose-effect above a daily intake of 125 g ethanol.

摘要

我们的目标是设计一种可重复的方法来测量肝硬化患者的终生酒精摄入量,并采用病例对照设计和多变量分析来评估与酒精摄入相关的肝失代偿风险。我们研究了439例失代偿期肝硬化患者(“病例组”)和233例代偿期肝硬化患者(“对照组”)。通过标准化问卷测量终生平均每日酒精摄入量和饮酒持续时间,通过对75名亲属进行访谈评估该问卷的可重复性,每日酒精摄入量的可重复性为70%,饮酒持续时间的可重复性为84%。在患者出院时再次访谈发现可重复性更好。男性、年轻患者和肝失代偿患者的每日酒精摄入量显著更高。根据终生平均每日酒精摄入量进行分层后,我们发现从每日摄入125克乙醇起,肝失代偿风险显著增加。未发现饮酒持续时间与肝失代偿风险之间存在关联。我们得出结论,酒精摄入量可以可靠且可重复地测量:在肝硬化患者中,酒精摄入量增加与肝失代偿风险增加相关,每日摄入超过125克乙醇时存在显著的剂量效应。

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