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乙醛修饰血红蛋白及其他慢性重度饮酒标志物的评估:性别和血红蛋白浓度的影响

Evaluation of acetaldehyde-modified hemoglobin and other markers of chronic heavy alcohol use: effects of gender and hemoglobin concentration.

作者信息

Hazelett S E, Liebelt R A, Brown W J, Androulakakis V, Jarjoura D, Truitt E B

机构信息

St. Thomas Medical Center, Summa Health System, Akron, Ohio, USA.

出版信息

Alcohol Clin Exp Res. 1998 Nov;22(8):1813-9.

PMID:9835301
Abstract

The present study examined whether measurement of hemoglobin-acetaldehyde (HbA1-AcH) using an improved methodology may be useful as a biological marker of alcohol abuse. Red blood cell hemolysates of 182 patients consecutively admitted to the drug and alcohol treatment unit of our institution were analyzed for HbA1-AcH concentration using cation exchange HPLC. Mean HbA1-AcH of those who claimed to drink > or = 6 drinks/day [mean = 0.055 (% total hemoglobin), SD = 0.051] was significantly higher than the mean of those who drank < 6 drinks/day (mean = 0.026, SD = 0.0174). The greatest sum of sensitivity (67%) and specificity (77%) came with a cut-score of 0.030 area% of total hemoglobin. A cut-score of 0.080 produced a 100% specificity, but lowered the sensitivity to 20%. The Pearson product moment correlation (r) between HbA1-AcH and reported drinks per day was r = 0.30 (p < 0.001). There was no significant difference in the association of HbA1-AcH and reported drinking between males and females, and the small difference observed was shown to be entirely associated with differences in hemoglobin levels between the sexes. Cocaine use did not significantly alter the correlation between reported drinking and HbA1-AcH levels. Hemoglobin levels were shown to have a significant correlation with HbA1-AcH independent of drinking. HbA1-AcH was shown to have a better sensitivity and specificity than gamma-glutamyltransferase, ALT, AST, or mean corpuscular volume in this population. The results suggest that HbA1-AcH may be a useful marker to help detect alcohol abuse, especially in populations where other markers have been shown to fail.

摘要

本研究探讨了采用改进方法测量血红蛋白 - 乙醛(HbA1 - AcH)是否可用作酒精滥用的生物学标志物。使用阳离子交换高效液相色谱法分析了我院药物与酒精治疗科连续收治的182例患者的红细胞溶血产物中的HbA1 - AcH浓度。声称每天饮酒≥6杯的患者的平均HbA1 - AcH(平均值 = 0.055(占总血红蛋白的百分比),标准差 = 0.051)显著高于每天饮酒<6杯的患者的平均值(平均值 = 0.026,标准差 = 0.0174)。总血红蛋白面积百分比的截断值为0.030时,敏感性(67%)和特异性(77%)之和最大。截断值为0.080时,特异性为100%,但敏感性降至20%。HbA1 - AcH与每日报告饮酒量之间的Pearson积矩相关系数(r)为r = 0.30(p < 0.001)。男性和女性在HbA1 - AcH与报告饮酒量的关联上无显著差异,观察到的微小差异完全与性别之间血红蛋白水平的差异相关。使用可卡因并未显著改变报告饮酒量与HbA1 - AcH水平之间的相关性。血红蛋白水平与HbA1 - AcH显示出独立于饮酒的显著相关性。在该人群中,HbA1 - AcH显示出比γ-谷氨酰转移酶、谷丙转氨酶、谷草转氨酶或平均红细胞体积更好的敏感性和特异性。结果表明,HbA1 - AcH可能是有助于检测酒精滥用的有用标志物,尤其是在已证明其他标志物无效的人群中。

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