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对人尿液中克仑特罗对映体组成的分析能否区分运动药物检测中克仑特罗的非法使用与食物污染?

Does the analysis of the enantiomeric composition of clenbuterol in human urine enable the differentiation of illicit clenbuterol administration from food contamination in sports drug testing?

机构信息

Center for Preventive Doping Research - Institute of Biochemistry, German Sport University Cologne, Cologne, Germany.

出版信息

Rapid Commun Mass Spectrom. 2013 Feb 28;27(4):507-12. doi: 10.1002/rcm.6485.

Abstract

RATIONALE

Clenbuterol (4-amino-α-[(tert-butylamino)methyl]-3,5-dichlorobenzyl alcohol) is approved for human and veterinary use primarily for the treatment of pulmonary afflictions. Despite the authorized administration in cases of medical indications, the misuse of clenbuterol in animal husbandry as well as elite and amateur sport has frequently been reported, arguably due to growth-promoting properties. Due to various recent incidences of doping control specimens containing clenbuterol, strategies towards the discrimination of a surreptitious application from unintended intake via animal-derived edibles or dietary supplements were required.

METHODS

The enantiomeric compositions of clenbuterol in human urine samples derived from administration studies with therapeutic amounts of the β(2)-agonist and authentic doping control specimens were determined. Due to the facts that therapeutic clenbuterol consists of a racemic mixture of (+)- and (-)-stereoisomers and that the first mentioned (dextrorotatory) stereoisomer is retained to a greater extent in edible animal tissue, the differentiation of a recent administration of therapeutic (and thus racemic) clenbuterol from food contamination (stereoisomerically depleted clenbuterol) was considered. Employing deuterated clenbuterol as internal standard, the target analytes were extracted from human urine by means of concerted liquid-liquid and solid-phase extractions and subjected to chiral liquid chromatography hyphenated to high resolution/high accuracy mass spectrometry with electrospray ionization.

RESULTS

Both enantiomers of clenbuterol were baseline separated and relative abundances of corresponding labeled and unlabeled stereoisomers were determined, demonstrating that the therapeutic use of clenbuterol results in racemic mixtures in urine for at least 24 h while adverse analytical findings presumably originating from food contaminations can yield (-)-clenbuterol-depleted pairs of analytes.

CONCLUSIONS

The determination of relative abundances of clenbuterol enantiomers can indicate the ingestion of clenbuterol via contaminated food; however, depletion of (-)-clenbuterol in edible animal tissue is time-dependent and thus results can still be inconclusive as to the inadvertent ingestion of clenbuterol when clenbuterol administration to animals was conducted until slaughter.

摘要

原理

克仑特罗(4-氨基-α-[(叔丁基)氨基甲基]-3,5-二氯苄醇)主要用于治疗肺部疾病,经批准可用于人类和兽医用途。尽管在有医疗指征的情况下可以进行授权管理,但在畜牧业以及精英和业余运动中,克仑特罗的滥用情况经常被报道,这可能是由于其具有促进生长的特性。由于最近兴奋剂控制样本中经常含有克仑特罗,因此需要制定策略来区分通过动物源性食品或膳食补充剂进行的秘密应用与非故意摄入。

方法

在具有治疗剂量β(2)-激动剂的人体尿液样本和真实的兴奋剂控制样本中,测定了克仑特罗的对映体组成。由于治疗用克仑特罗由(+)-和(-)-对映异构体的外消旋混合物组成,并且第一种(右旋)对映异构体在食用动物组织中保留的程度更大,因此考虑了从食物污染(对映体耗尽的克仑特罗)中区分最近给予的治疗(因此是外消旋)克仑特罗。采用氘代克仑特罗作为内标,通过协同液-液和固相萃取从人尿中提取目标分析物,并进行手性液相色谱-高分辨率/高精度质谱联用分析,采用电喷雾电离。

结果

克仑特罗的两种对映异构体均实现基线分离,并确定了相应标记和未标记对映异构体的相对丰度,证明至少在 24 小时内,治疗用克仑特罗在尿液中产生外消旋混合物,而来自食物污染的不利分析结果可能导致 (-)-克仑特罗耗尽的分析物对。

结论

克仑特罗对映体的相对丰度的测定可以表明通过受污染的食物摄入克仑特罗;然而,食用动物组织中 (-)-克仑特罗的耗尽是时间依赖性的,因此当动物给药直至屠宰时,结果仍然不能确定是否无意中摄入了克仑特罗。

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