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Differentially methylated Embryonal Fyn-associated Substrate (EFS) gene as a blood-specific epigenetic marker and its potential application in forensic casework

机译:差异甲基化的胚胎Fyn相关基质(EFS)基因作为血液特异性表观遗传标记及其在法医案例研究中的潜在应用

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摘要

DNA methylation patterns have the ability to reveal the activities of genes within a certain tissue at a particular time point. Tissue-specific DNA methylation patterns have been previously investigated for their applicability in the identification of forensically relevant body fluids, however there is still a lack in robust markers. While following a genome-wide scale investigation has a great potential to reveal useful tissue-specific changes, a gene-targeted approach can also lead to significant outcomes, especially in genomic locations not included in the genome-wide experiments. In this study, the potential of the candidate embryonal Fyn-associated substrate (EFS) gene for the positive identification of whole blood was investigated. For this purpose, the methylation profile of a selected genomic region containing a total of 10 CpG sites was analysed in 124 individuals via bisulfite pyrosequencing. Volunteers donated various forensically relevant tissues, including whole blood, saliva, seminal fluid, vaginal fluid and menstrual secretion. Whole blood showed the highest levels of DNA methylation (mean = 0.67), while semen samples were found to be very low methylated (mean = 0.06). The remaining tissues demonstrated partial mean methylation levels; more specifically, saliva − 0.43, vaginal fluid − 0.22 and menstrual blood − 0.22. One out of the 10 analysed CpG sites, CpG4, showed to be more robust, resulting in not only the highest methylation difference between blood and the rest of the tissues, but also the lowest inter-individual methylation difference. The proposed pyrosequencing assay was found to be accurate, linear and reproducible. Lastly, the method’s applicability to forensic casework was assessed via the analysis of very old bloodstains stored up to 18 years, blood DNA samples stored long-term up to 9 years, mixed stains as well as other ‘forensic-like’ samples. In the majority of cases the expected methylation ratios were obtained indicating a stable DNA methylation pattern, however caution is necessary when analysing low quantity and/or quality samples due to potential stochastic effects. Future validation experiments can shed more light into the usefulness of EFS locus as a promising blood-specific epigenetic marker.
机译:DNA甲基化模式具有在特定时间点揭示特定组织内基因活动的能力。先前已经研究了组织特异性DNA甲基化模式在鉴定法医相关体液中的适用性,但是仍然缺乏可靠的标记。尽管进行全基因组规模的研究具有揭示有用的组织特异性变化的巨大潜力,但是以基因为靶标的方法也可以产生重要的结果,尤其是在全基因组实验未包括的基因组位置。在这项研究中,研究了候选胚胎Fyn相关底物(EFS)基因对全血阳性鉴定的潜力。为此,通过亚硫酸氢盐焦磷酸测序法分析了124个个体中包含总共10个CpG位点的选定基因组区域的甲基化谱。志愿者捐赠了各种法医相关组织,包括全血,唾液,精液,阴道液和月经分泌物。全血显示出最高的DNA甲基化水平(平均值= 0.67),而精液样本的甲基化水平非常低(平均值= 0.06)。其余组织显示出部分平均甲基化水平。更具体地说,唾液-0.43,阴道液-0.22和经血-0.22。在分析的10个CpG位点中,有1个CpG4具有更强的鲁棒性,不仅导致血液与其余组织之间的甲基化差异最高,而且各个个体之间的甲基化差异最低。发现所提出的焦磷酸测序测定法是准确,线性和可重复的。最后,通过分析长达18年的非常旧的血迹,长期保存9年的血液DNA样本,混合污渍以及其他“法医样”样本,评估了该方法在法医案例研究中的适用性。在大多数情况下,获得了预期的甲基化率,表明DNA甲基化模式稳定,但是在分析少量和/或高质量样品时,由于潜在的随机效应,必须格外小心。未来的验证实验可以为EFS基因位点作为有希望的血液特异性表观遗传标记的有用性提供更多的线索。

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