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Comparison of the Allelic Alterations between InDel and STR Markers in Tumoral Tissues Used for Forensic Purposes

机译:用于法医用途的肿瘤组织中吲哚和str标记的等位基因改变的比较

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摘要

Background and objectives: Over the last two decades, human DNA identification and kinship tests have been conducted mainly through the analysis of short tandem repeats (STRs). However, other types of markers, such as insertion/deletion polymorphisms (InDels), may be required when DNA is highly degraded. In forensic genetics, tumor samples may sometimes be used in some cases of human DNA identification and in paternity tests. Nevertheless, tumor genomic instability related to forensic DNA markers should be considered in forensic analyses since it can compromise genotype attribution. Therefore, it is useful to know what impact tumor transformation may have on the forensic interpretation of the results obtained from the analysis of these polymorphisms. Materials and Methods: The aim of this study was to investigate the genomic instability of InDels and STRs through the analysis of 55 markers in healthy tissue and tumor samples (hepatic, gastric, breast, and colorectal cancer) in 66 patients. The evaluation of genomic instability was performed comparing InDel and STR genotypes of tumor samples with those of their healthy counterparts. Results: With regard to STRs, colorectal cancer was found to be the tumor type affected by the highest number of mutations, whereas in the case of InDels the amount of genetic mutations turned out to be independent of the tumor type. However, the phenomena of genomic instability, such as loss of heterozygosity (LOH) and microsatellite instability (MSI), seem to affect InDels more than STRs hampering genotype attribution. Conclusion: We suggest that the use of STRs rather than InDels could be more suitable in forensic genotyping analyses given that InDels seem to be more affected than STRs by mutation events capable of compromising genotype attribution.
机译:背景和目标:在过去二十年中,通过对短串联重复(STRS)的分析,主要通过分析来进行人体DNA鉴定和亲属试验。然而,当DNA高度降解时,可能需要其他类型的标记,例如插入/缺失多态性(吲哚)。在法医遗传学中,肿瘤样品有时可以在某些人DNA鉴定和亲子鉴定中使用。然而,与法医DNA标记相关的肿瘤基因组不稳定性应考虑在法医分析中,因为它可以危及基因型归因。因此,了解肿瘤转化可能对从这些多态性分析的分析中获得的结果的法医解释是有用的。材料和方法:本研究的目的是通过分析66例患者的健康组织和肿瘤样品(肝,胃,乳腺癌和结直肠癌)的55种标记来研究吲哚和strs的基因组不稳定性。对基因组不稳定性的评估进行了与健康对应物的肿瘤样品的吲哚和str基因型进行了比较。结果:关于STRS,发现结直肠癌是受突变数量影响影响的肿瘤类型,而在诱导的情况下,遗传突变的量却与肿瘤类型无关。然而,基因组不稳定性的现象,例如杂合性丧失(LOH)和微卫星不稳定性(MSI),似乎比妨碍基因型归因的诱惑程度大。结论:我们建议使用strs而不是诱导可能更适合法医基因分析分析,因为诱导似乎受到能够损害基因型归因的突变事件的突变事件的影响。

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