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首页> 外文期刊>Animal Genetics >Whole genome sequencing reveals a novel deletion variant in the KIT gene in horses with white spotted coat colour phenotypes
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Whole genome sequencing reveals a novel deletion variant in the KIT gene in horses with white spotted coat colour phenotypes

机译:全基因组测序揭示了具有白色斑点涂层颜色表型的马匹中的KIT基因中的新型删除变体

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摘要

White spotting phenotypes in horses can range in severity from the common white markings up to completely white horses. EDNRB, KIT, MITF, PAX3 and TRPM1 represent known candidate genes for such phenotypes in horses. For the present study, we re-investigated a large horse family segregating a variable white spotting phenotype, for which conventional Sanger sequencing of the candidate genes' individual exons had failed to reveal the causative variant. We obtained whole genome sequence data from an affected horse and specifically searched for structural variants in the known candidate genes. This analysis revealed a heterozygous similar to 1.9-kb deletion spanning exons 10-13 of the KIT gene (chr3:77,740,239_77,742,136del1898insTATAT). In continuity with previously named equine KIT variants we propose to designate the newly identified deletion variant W22. We had access to 21 horses carrying the W22 allele. Four of them were compound heterozygous W20/W22 and had a completely white phenotype. Our data suggest that W22 represents a true null allele of the KIT gene, whereas the previously identified W20 leads to a partial loss of function. These findings will enable more precise genetic testing for depigmentation phenotypes in horses.
机译:马匹的白色斑点表型可以从普通的白色标记到完全白马的严重程度。 EDNRB,试剂盒,MITF,PAX3和TRPM1代表了马匹中这种表型的已知候选基因。对于目前的研究,我们重新调查了一种大的马家族,这些大型马族分离可变白色斑点表型,候选基因的常规Sanger序列的个体外显子未能揭示致病变异。我们从受影响的马中获得全基因组序列数据,并专门搜索已知候选基因中的结构变体。该分析显示了杂合,类似于KIT基因的1.9-kB缺失跨越外显子10-13(CHR3:77,740,239_77,742,136del1898instatat)。在与以前命名的标准套件变体的连续性中,我们建议指定新识别的删除变体W22。我们可以使用携带W22等位基因的21匹马。其中四个是化合物杂合的W20 / W22,并且具有完全白色的表型。我们的数据表明W22代表了试剂盒基因的真正无效等位基因,而先前识别的W20会导致功能的部分损失。这些发现将使马匹中的脱毛表型更精确的遗传测试。

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