Comprehensive genetic testing combined with citizen science reveals a recently characterized ancient MC1R mutation associated with partial recessive red phenotypes in dog.

Heidi Anderson, Leena Honkanen, Päivi Ruotanen, Julia Mathlin, Jonas Donner
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引用次数: 8

Abstract

Background: The Melanocortin 1 Receptor (MC1R) plays a central role in regulation of coat color determination in various species and is commonly referred to as the "E (extension) Locus". Allelic variation of the MC1R gene is associated with coat color phenotypes EM (melanistic mask), EG (grizzle/domino) and e1-3 (recessive red) in dogs. In addition, a previous study of archeological dog specimens over 10,000 years of age identified a variant p.R301C in the MC1R gene that may have influenced coat color of early dogs.

Results: Commercial genotyping of 11,750 dog samples showed the R301C variant of the MC1R gene was present in 35 breeds or breed varieties, at an allele frequency of 1.5% in the tested population. We detected no linkage disequilibrium between R301C and other tested alleles of the E locus. Based on current convention we propose that R301C should be considered a novel allele of the E locus, which we have termed eA for "e ancient red". Phenotype analysis of owner-provided dog pictures reveals that the eA allele has an impact on coat color and is recessive to wild type E and dominant to the e alleles. In dominant black (KB/*) dogs it can prevent the phenotypic expression of the K locus, and the expressed coat color is solely determined by the A locus. In the absence of dominant black, eA/eA and eA/e genotypes result in the coat color patterns referred to in their respective breed communities as domino in Alaskan Malamute and other Spitz breeds, grizzle in Chihuahua, and pied in Beagle.

Conclusions: This study demonstrates a large genotype screening effort to identify the frequency and distribution of the MC1R R301C variant, one of the earliest mutations captured by canine domestication, and citizen science empowered characterization of its impact on coat color.

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综合基因检测结合公民科学揭示了最近表征的古代MC1R突变与狗的部分隐性红色表型相关。
背景:黑素皮质素1受体(Melanocortin 1 Receptor, MC1R)在多种动物的毛色决定调控中起着核心作用,通常被称为“E(延伸)位点”。MC1R基因的等位基因变异与狗的毛色表型EM(黑面具)、EG(灰褐色/多米诺骨牌)和e1-3(隐性红色)有关。此外,之前对一万多年前的考古狗标本的研究发现,MC1R基因中的p.R301C变异可能影响了早期狗的毛色。结果:11750只狗的商业基因分型显示,35个品种或品种中存在MC1R基因的R301C变异,等位基因频率为1.5%。我们未发现R301C与E位点其他被测等位基因之间的连锁不平衡。根据目前的惯例,我们建议R301C应该被认为是E位点的一个新的等位基因,我们将其称为eA,即“E古红”。对主人提供的狗照片进行表型分析表明,eA等位基因对毛色有影响,对野生型E隐性,对E等位基因显性。在显性黑犬(KB/*)中,它可以阻止K位点的表型表达,表达的毛色完全由A位点决定。在没有显性黑色的情况下,eA/eA和eA/e基因型导致了各自品种群体中被称为多米诺骨牌的阿拉斯加雪橇犬和其他斯皮兹品种,奇瓦瓦犬的灰色,比格犬的斑纹。结论:本研究展示了大量的基因型筛选工作,以确定MC1R R301C变异的频率和分布,这是犬驯化中最早发现的突变之一,公民科学授权表征其对毛色的影响。
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