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鉴定绵羊朊病毒蛋白(SPRN)基因中的多态性,并评估其对启动子活性和经典瘙痒病易感性的影响。

Identification of polymorphisms in the ovine Shadow of prion protein (SPRN) gene and assessment of their effect on promoter activity and susceptibility for classical scrapie.

机构信息

Department of Nutrition, Genetics and Ethology, Ghent University, Merelbeke, Belgium.

出版信息

Anim Genet. 2010 Apr;41(2):169-78. doi: 10.1111/j.1365-2052.2009.01984.x. Epub 2009 Nov 16.

DOI:10.1111/j.1365-2052.2009.01984.x
PMID:19917049
Abstract

Shadow of prion protein (SPRN) is an interesting candidate gene thought to be involved in prion pathogenesis. In humans, an association has already been discovered between mutations in SPRN and the incidence of variant and sporadic Creutzfeldt-Jakob disease. However, in sheep, the effect of mutations in SPRN is largely unknown. Therefore, we analysed the presence of mutations in the entire ovine SPRN gene, their association with scrapie susceptibility and their effect on SPRN promoter activity. In total, 26 mutations were found: seven in the promoter region, four in intron 1, seven in the coding sequence and eight in the 3' untranslated region. The mutations detected in the coding sequence and the promoter region were subsequently analysed in more detail. In the coding sequence, a polymorphism causing a deletion of two alanines was found to be associated with susceptibility for classical scrapie in sheep. Furthermore, a functional analysis of deletion constructs of the ovine SPRN promoter revealed that the region 464 to 230 bp upstream of exon 1 (containing a putative AP-2 and putative Sp1 binding sites) is of functional importance for SPRN transcription. Six mutations in the SPRN promoter were also found to alter the promoter activity in vitro. However, no association between any of these promoter mutations and susceptibility for classical scrapie was found.

摘要

朊病毒蛋白(Prion protein,PRNP)的阴影(Shadow of prion protein,SPRN)是一个有趣的候选基因,被认为与朊病毒发病机制有关。在人类中,已经发现 SPRN 突变与变异型和散发性克雅氏病的发生之间存在关联。然而,在绵羊中,SPRN 突变的影响在很大程度上尚不清楚。因此,我们分析了绵羊 SPRN 基因的整个基因中突变的存在、它们与瘙痒病易感性的关联以及它们对 SPRN 启动子活性的影响。总共发现了 26 个突变:7 个位于启动子区域,4 个位于内含子 1,7 个位于编码序列,8 个位于 3'非翻译区。随后对编码序列和启动子区域中检测到的突变进行了更详细的分析。在编码序列中,发现了一个导致两个丙氨酸缺失的多态性,与绵羊经典瘙痒病的易感性有关。此外,对绵羊 SPRN 启动子缺失构建体的功能分析表明,外显子 1 上游 464 至 230bp 区域(包含一个假定的 AP-2 和假定的 Sp1 结合位点)对 SPRN 转录具有功能重要性。在 SPRN 启动子中还发现了 6 个突变,它们改变了体外的启动子活性。然而,没有发现这些启动子突变与经典瘙痒病易感性之间存在任何关联。

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