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法医STR作为潜在的疾病标志物:血管性血友病因子基因座(VWA)与血管性血友病的研究

Forensic STRs as potential disease markers: a study of VWA and von Willebrand's Disease.

作者信息

Laird Rebecca, Schneider Peter M, Gaudieri Silvana

机构信息

Centre for Forensic Science, University of Western Australia, Nedlands, Western Australia, Australia.

出版信息

Forensic Sci Int Genet. 2007 Dec;1(3-4):253-61. doi: 10.1016/j.fsigen.2007.06.002. Epub 2007 Jul 13.

Abstract

In recent years it has been established that non-coding variants may be in linkage disequilibrium (LD) with coding variants up to several thousand base pairs away forming haplotype blocks. These non-coding markers may be haplotype specific and, therefore, informative regarding the surrounding coding sequence. In this study, we chose to study the VWA short tandem repeat (STR) as it is targeted in all major commercial kits utilized in routine forensic DNA profiling and is located in the von Willebrand Factor (vWF) gene; a gene associated with von Willebrand's Disease (vWD). We examined the VWA STR together with single nucleotide polymorphisms (SNPs) located throughout the vWF gene to identify haplotype structures and the extent of LD between markers in the region. Several areas exhibiting LD were identified by population data analysis in the 178 kilobase (178 kb) vWF gene, which was supported by family studies. However, there appeared to be no evidence of LD blocks surrounding the VWA STR and evidence for recombination within 3 kb of VWA, hence, it is unlikely that VWA STR alleles could be used to predict haplotypes within the vWF gene that are associated with different forms of vWD.

摘要

近年来已经确定,非编码变异可能与数千个碱基对以外的编码变异处于连锁不平衡(LD)状态,从而形成单倍型块。这些非编码标记可能具有单倍型特异性,因此,对于周围的编码序列具有信息价值。在本研究中,我们选择研究VWA短串联重复序列(STR),因为它是常规法医DNA分型中所有主要商业试剂盒的靶向序列,并且位于血管性血友病因子(vWF)基因中;该基因与血管性血友病(vWD)相关。我们将VWA STR与位于整个vWF基因中的单核苷酸多态性(SNP)一起进行检测,以确定单倍型结构以及该区域内标记之间的LD程度。通过对178千碱基(178 kb)vWF基因的群体数据分析确定了几个显示LD的区域,家族研究也支持这一结果。然而,似乎没有证据表明VWA STR周围存在LD块,也没有证据表明VWA 3 kb范围内发生重组,因此,VWA STR等位基因不太可能用于预测vWF基因内与不同形式vWD相关的单倍型。

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