首页> 外文期刊>Genomics >Linkage disequilibrium mapping in domestic dog breeds narrows the progressive rod-cone degeneration interval and identifies ancestral disease-transmitting chromosome.
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Linkage disequilibrium mapping in domestic dog breeds narrows the progressive rod-cone degeneration interval and identifies ancestral disease-transmitting chromosome.

机译:家犬品种中的连锁不平衡作图缩小了渐进的杆锥变性间隔并鉴定了传承疾病的染色体。

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摘要

Canine progressive rod-cone degeneration (prcd) is a retinal disease previously mapped to a broad, gene-rich centromeric region of canine chromosome 9. As allelic disorders are present in multiple breeds, we used linkage disequilibrium (LD) to narrow the approximately 6.4-Mb interval candidate region. Multiple dog breeds, each representing genetically isolated populations, were typed for SNPs and other polymorphisms identified from BACs. The candidate region was initially localized to a 1.5-Mb zero recombination interval between growth factor receptor-bound protein 2 (GRB2) and SEC14-like 1 (SEC14L). A fine-scale haplotype of the region was developed, which reduced the LD interval to 106 kb and identified a conserved haplotype of 98 polymorphisms present in all prcd-affected chromosomes from 14 different dog breeds. The findings strongly suggest that a common ancestor transmitted the prcd disease allele to many of the modern dog breeds and demonstrate the power of the LD approach in the canine model.
机译:犬进行性杆状圆锥变性(prcd)是一种先前定位于犬9号染色体上广泛的,基因丰富的着丝粒区域的视网膜疾病。由于等位基因疾病存在于多个品种中,因此我们使用连锁不平衡(LD)缩小了大约6.4的范围。 -Mb间隔候选区域。根据从BAC中鉴定出的SNP和其他多态性,对每个代表遗传分离种群的多个犬种进行了分类。候选区域最初位于生长因子受体结合蛋白2(GRB2)和SEC14-like 1(SEC14L)之间的1.5 Mb零重组间隔。开发了该区域的精细单倍型,其将LD间隔降低至106 kb,并鉴定了来自14种不同犬种的所有受prcd影响的染色体中存在的98个多态性的保守单倍型。这些发现强烈表明,一个共同的祖先将prcd疾病等位基因传播给了许多现代犬种,并证明了犬模型中LD方法的强大作用。

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