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使用海洛因的司机:吗啡和吗啡-6-葡萄糖醛酸对晚期临床损伤的重要性。

Heroin-using drivers: importance of morphine and morphine-6-glucuronide on late clinical impairment.

作者信息

Bachs Liliana, Høiseth Gudrun, Skurtveit Svetlana, Mørland Jørg

机构信息

Division for Forensic Toxicology and Drug Abuse, Norwegian Institute of Public Health, P.O. Box 4404, Nydalen, 0403, Oslo, Norway.

出版信息

Eur J Clin Pharmacol. 2006 Nov;62(11):905-12. doi: 10.1007/s00228-006-0195-y. Epub 2006 Oct 5.

DOI:10.1007/s00228-006-0195-y
PMID:17021891
Abstract

OBJECTIVE

To evaluate the relationship between major heroin metabolites (morphine, morphine-6-glucoronide), pattern of drug use, and late impairment of psychomotor functions.

METHODS

From the database of the Norwegian Institute of Public Health, Oslo, blood morphine concentration in samples from heroin users (n=70) containing only morphine were correlated with results of the clinical test for impairment (CTI). For comparison, test results were explored in individuals without any positive analytical finding in blood samples (n=79) selected from the same database.

RESULTS

In the "no drug" cases, 86% were judged as not impaired and 14% as impaired. In the morphine only cases, 20% were judged as not impaired, and 80% as impaired. Both daily users and non-daily users had the same proportion of impaired cases. Median blood morphine concentration (M) was 0.09 micromol/l in the "not impaired" group and 0.15 micromol/l in the "impaired" group (P=0.067). For morphine-6-glucuronide (M6G), the median blood concentration was 0.09 micromol/l in the "not impaired" group and 0.14 micromol/l in the "impaired" group (P=0.030). A significant correlation between concentration quartiles and number of cases determined as "impaired" was found for M6G (P=0.018) and for the sum M+M6G (P=0.013).

CONCLUSION

In our population of heroin-drugged drivers, blood concentrations of M6G and the sum M+M6G appeared to have concentration-dependent effects on the CNS that may lead to impairment as judged from a CTI. Variations in pattern of use did not seem to have any bearing on the judgement of impairment.

摘要

目的

评估主要海洛因代谢物(吗啡、吗啡 - 6 - 葡萄糖醛酸苷)、用药模式与精神运动功能晚期损害之间的关系。

方法

从奥斯陆挪威公共卫生研究所的数据库中,将仅含有吗啡的海洛因使用者样本(n = 70)中的血吗啡浓度与损害临床测试(CTI)结果进行关联。为作比较,在从同一数据库中选取的血样无任何阳性分析结果的个体(n = 79)中探究测试结果。

结果

在“未用药”病例中,86%被判定未受损,14%被判定受损。在仅使用吗啡的病例中,20%被判定未受损,80%被判定受损。每日使用者和非每日使用者的受损病例比例相同。“未受损”组的血吗啡浓度中位数(M)为0.09微摩尔/升,“受损”组为0.15微摩尔/升(P = 0.067)。对于吗啡 - 6 - 葡萄糖醛酸苷(M6G),“未受损”组的血浓度中位数为0.09微摩尔/升,“受损”组为0.14微摩尔/升(P = 0.030)。发现M6G(P = 0.018)以及M + M6G总和(P = 0.013)的浓度四分位数与被判定为“受损”的病例数之间存在显著相关性。

结论

在我们的海洛因成瘾驾驶者群体中,M6G以及M + M6G总和的血浓度似乎对中枢神经系统具有浓度依赖性影响,从CTI判断可能导致损害。用药模式的差异似乎对损害判断没有任何影响。

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