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用于鉴定“接触性 DNA”证据中皮肤的特异性和灵敏性 mRNA 生物标志物。

Specific and sensitive mRNA biomarkers for the identification of skin in 'touch DNA' evidence.

机构信息

National Center for Forensic Science, PO Box 162367, Orlando, FL 32816-2367, USA.

出版信息

Forensic Sci Int Genet. 2012 Sep;6(5):548-58. doi: 10.1016/j.fsigen.2012.01.004. Epub 2012 Feb 9.

Abstract

In forensic casework analysis it is often necessary to attempt to obtain DNA profiles from microscopic amounts of biological material left behind by perpetrators of crime. The ability to obtain profiles from trace biological evidence is routinely demonstrated with so-called 'touch DNA' evidence, which is generally perceived to be the result of DNA obtained from shed skin cells transferred from donor to an object or person during physical contact. Although a genetic profile from trace biological evidence is routinely obtained, the tissue source of the profile is rarely known. This merely perpetuates the 'mystery' of the nature of 'touch DNA' evidence allowing the significance or meaningfulness of genetic profiles obtained from these samples to be challenged. Numerous reports state that the tissue source of origin of 'touch DNA' evidence cannot be determined due to the small amount of biological material present, while others conclude that the DNA profiles are obtained from shed skin cells (as opposed to, say, buccal epithelial cells present in saliva traces) without any scientific basis for this assertion. Proper identification of the biological material present might be crucial to the investigation and prosecution of a criminal offense and a misrepresentation of the nature of the evidence can have undue influence on the perception of the circumstance of the crime. Thus far, research has failed to provide forensic scientists with feasible, definitive methods to identify the tissue origin of 'touch DNA'. In the present work, we sought to identify novel highly specific and sensitive messenger RNA (mRNA) biomarkers for the identification of skin. Gene candidates were identified using both literature searches and whole transcriptome deep sequencing (RNA-Seq). Utilizing this dual approach, we identified and evaluated over 100 gene candidates. Five mRNA markers were identified that demonstrated a high degree of specificity for skin. Using these markers, we have been able to successfully detect and identify skin using as little as 5-25 pg of input total RNA from skin and, significantly, in swabs of human skin and various touched objects. One of the markers, LCE1C, is particularly highly sensitive and was detected in the majority of skin samples tested including touched objects. We have been successful in incorporating the five skin biomarkers into two multiplex systems. Although further work is needed to optimize the assay for routine casework, the initial studies demonstrate that a molecular-based characterization of the biological material recovered from touch samples is possible.

摘要

在法医案件分析中,通常需要尝试从犯罪行为留下的微量生物材料中获取 DNA 图谱。从所谓的“接触 DNA”证据中获取图谱的能力通常是通过常规手段证明的,这种证据通常被认为是从供体转移到物体或人身上的脱落皮肤细胞中获得的 DNA。尽管可以从痕量生物证据中常规获得遗传图谱,但很少知道该图谱的组织来源。这仅仅延续了“接触 DNA”证据性质的“神秘性”,从而使从这些样本中获得的遗传图谱的意义或重要性受到质疑。许多报告指出,由于存在的生物材料量很少,无法确定“接触 DNA”证据的组织来源,而其他报告则得出结论,DNA 图谱是从脱落的皮肤细胞中获得的(而不是从唾液痕迹中存在的口腔上皮细胞等中获得),而没有任何科学依据支持这一说法。正确识别存在的生物材料对于犯罪调查和起诉可能至关重要,而对证据性质的错误表述可能会对犯罪情况的认知产生不当影响。迄今为止,研究未能为法医科学家提供可行的、明确的方法来识别“接触 DNA”的组织来源。在本工作中,我们试图确定用于识别皮肤的新型高度特异和敏感的信使 RNA(mRNA)生物标志物。使用文献检索和全转录组深度测序(RNA-Seq)两种方法来鉴定候选基因。利用这种双重方法,我们鉴定和评估了 100 多个候选基因。鉴定出 5 个具有高度皮肤特异性的 mRNA 标志物。使用这些标记物,我们已经能够成功地检测和识别出 5-25pg 输入总 RNA 的皮肤,并且重要的是,能够在人体皮肤和各种接触物体的拭子中检测到皮肤。其中一个标记物 LCE1C 特别敏感,在测试的大多数皮肤样本中都能检测到,包括接触物体。我们已经成功地将这 5 个皮肤生物标志物整合到两个多重系统中。尽管需要进一步的工作来优化常规案例工作的测定,但初步研究表明,从接触样本中回收的生物材料的分子特征是可能的。

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