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首页> 外文期刊>International Journal of Legal Medicine >Toxicogenetics—cytochrome P450 microarray analysis in forensic cases focusing on morphine/codeine and diazepam
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Toxicogenetics—cytochrome P450 microarray analysis in forensic cases focusing on morphine/codeine and diazepam

机译:毒理遗传学—法医病例中的细胞色素P450微阵列分析,重点是吗啡/可待因和地西epa

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Genetic polymorphisms in cytochrome P 450 (CYP) enzymes could lead to a phenotype with altered enzyme activity. In pharmacotherapy, genotype-based dose recommendations achieved great importance for several drugs. In our pilot study, we ask if these genetic tests should be applied to forensic problems as a matter of routine. Starting from 2004 through 2008, we screened routine cases for samples where the relation of parent compound to metabolite(s) (P/M ratio), particularly morphine to codeine ratios and diazepam to its metabolites, was noticeable or not consistent with the information provided by the defendants. We found 11 samples with conspicuous results. These were analyzed for polymorphisms of the CYP 2D6 and 2C19 genes using the Roche AmpliChip Cytochrome P450 Genotyping test. If not previously conducted, a general unknown analysis by gas chromatography/mass spectrometry (GC/MS) was additionally carried out. For CYP 2D6, we found two cases with the genotype poor metabolizer (PM), three cases with heterozygote extensive metabolizer genotype classified as an intermediate metabolizer (IM) with probably reduced enzyme activities, but no ultrarapid metabolizer genotype. For CYP 2C19, two cases were characterized as IM phenotypes, with no PM found. Once we achieved no appropriate amounts of DNA, one case was excluded after GC/MS analysis. Only in one case could the polymorphism clearly explain the changes in drug metabolism. More frequently, a drug–drug interaction was thought to have a stronger impact. Additionally, our results suggest that IM genotypes may be more relevant than previously suspected. With respect to the small number of cases in which we thought a genotyping would be helpful, we conclude that the overall relevance of toxicogenetics in forensic problems is moderate. However, in some individual cases, a genotyping may provide new insight.
机译:细胞色素P 450(CYP)酶的遗传多态性可能导致酶活性改变的表型。在药物治疗中,基于基因型的剂量推荐对于几种药物非常重要。在我们的初步研究中,我们询问是否应将这些基因检测作为常规方法应用于法医问题。从2004年到2008年,我们筛选了例行病例的样本,这些样本中母体化合物与代谢产物(P / M比率)的关系,特别是吗啡对可待因比率以及地西epa与其代谢产物的关系明显或与提供的信息不一致被告。我们发现了11个样本,具有明显的结果。使用Roche AmpliChip细胞色素P450基因分型测试分析了CYP 2D6和2C19基因的多态性。如果以前没有进行过,则还需要通过气相色谱/质谱(GC / MS)进行一般未知的分析。对于CYP 2D6,我们发现2例基因型不良代谢者(PM),3例杂合子广泛代谢者基因型被分类为中间代谢物(IM),其酶活性可能降低,但没有超快速代谢者基因型。对于CYP 2C19,有2例以IM表型为特征,未发现PM。一旦我们没有获得适当量的DNA,GC / MS分析后将排除一例。只有在一种情况下,多态性才能清楚地解释药物代谢的变化。人们更经常地认为,药物之间的相互作用会产生更大的影响。此外,我们的结果表明IM基因型可能比以前怀疑的更相关。关于少数我们认为进行基因分型会有所帮助的案例,我们得出结论,毒物遗传学与法医问题的总体相关性是中等的。但是,在某些情况下,基因分型可能会提供新的见解。

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