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采用气相色谱-质谱联用法定量测定血清和尿液中的葡萄糖醛酸乙酯。

Quantitation of ethyl glucuronide in serum & urine by gas chromatography - mass spectrometry.

作者信息

Sharma Priyamvada, Bharat Venkatesh, Murthy Pratima

机构信息

Centre for Addiction Medicine, Department of Psychiatry, National Institute of Mental Health & Neuro Sciences, Bengaluru, India.

出版信息

Indian J Med Res. 2015 Jan;141(1):75-80. doi: 10.4103/0971-5916.154507.

Abstract

BACKGROUND & OBJECTIVES: Alcohol misuse has now become a serious public health problem and early intervention is important in minimizing the harm. Biochemical markers of recent and high levels of alcohol consumption can play an important role in providing feedback regarding the health consequences of alcohol misuse. Existing markers are not sensitive to recent consumption and in detecting early relapse. Ethyl glucuronide (EtG), a phase-II metabolite of ethanol is a promising marker of recent alcohol use and can be detected in body fluids. In this study an analytical technique for quantitation of EtG in body fluids using solid-phase extraction (SPE) and gas chromatography (GC) with mass spectrometric detection (MS) was developed and validated.

METHODS

De-proteinization of serum and urine samples was done with perchloric acid and hydrochloric acid, respectively. Serum samples were passed through phospholipids removal cartridges for further clean up. EtG was isolated using amino propyl solid phase extraction columns. Chromatographic separation was achieved by gas chromatography with mass spectrometry.

RESULTS

Limit of detection and limit of quantitation were 50 and 150 ng/ml for urine and 80 and 210 ng/ml for serum, respectively. Signal to noise ratio was 3:1, mean absolute recovery was 80-85 per cent. Significant correlation was obtained between breath alcohol and serum EtG levels (r=0.853) and urine EtG and time since last abuse (r = -0.903) in clinical samples.

INTERPRETATION & CONCLUSIONS: In the absence of other standardized techniques to quantitate EtG in biological samples, this gc - ms method was found to have high throughput and was sensitive and specific.

摘要

背景与目的

酒精滥用现已成为一个严重的公共卫生问题,早期干预对于将危害降至最低至关重要。近期大量饮酒的生化标志物在提供酒精滥用对健康影响的反馈方面可发挥重要作用。现有的标志物对近期饮酒情况不敏感,也难以检测早期复发。乙醇的Ⅱ相代谢产物葡糖醛酸乙酯(EtG)是近期饮酒的一个有前景的标志物,可在体液中检测到。在本研究中,开发并验证了一种使用固相萃取(SPE)和气相色谱(GC)结合质谱检测(MS)对体液中EtG进行定量的分析技术。

方法

血清和尿液样本分别用高氯酸和盐酸进行去蛋白处理。血清样本通过去除磷脂的柱进行进一步净化。使用氨基丙基固相萃取柱分离EtG。通过气相色谱 - 质谱联用实现色谱分离。

结果

尿液的检测限和定量限分别为50 ng/ml和150 ng/ml,血清的检测限和定量限分别为80 ng/ml和210 ng/ml。信噪比为3:1,平均绝对回收率为80 - 85%。临床样本中,呼气酒精含量与血清EtG水平之间(r = 0.853)以及尿液EtG与上次饮酒后时间之间(r = -0.903)存在显著相关性。

解读与结论

在缺乏其他标准化技术对生物样本中的EtG进行定量的情况下,发现这种气相色谱 - 质谱法具有高通量,且灵敏、特异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f4a/4405944/fc6967c81a6a/IJMR-141-75-g001.jpg

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