Animal Genomics Laboratory, School of Agriculture, Food Science and Veterinary Medicine, University College Dublin, Belfield, Dublin 4, Ireland.
BMC Genomics. 2010 Oct 11;11:552. doi: 10.1186/1471-2164-11-552.
Thoroughbred horses have been selected for traits contributing to speed and stamina for centuries. It is widely recognized that inherited variation in physical and physiological characteristics is responsible for variation in individual aptitude for race distance, and that muscle phenotypes in particular are important.
A genome-wide SNP-association study for optimum racing distance was performed using the EquineSNP50 Bead Chip genotyping array in a cohort of n = 118 elite Thoroughbred racehorses divergent for race distance aptitude. In a cohort-based association test we evaluated genotypic variation at 40,977 SNPs between horses suited to short distance (≤ 8 f) and middle-long distance (> 8 f) races. The most significant SNP was located on chromosome 18: BIEC2-417495 ~690 kb from the gene encoding myostatin (MSTN) [P(unadj.) = 6.96 x 10⁻⁶]. Considering best race distance as a quantitative phenotype, a peak of association on chromosome 18 (chr18:65809482-67545806) comprising eight SNPs encompassing a 1.7 Mb region was observed. Again, similar to the cohort-based analysis, the most significant SNP was BIEC2-417495 (P(unadj.) = 1.61 x 10⁻⁹; P(Bonf.) = 6.58 x 10⁻⁵). In a candidate gene study we have previously reported a SNP (g.66493737C>T) in MSTN associated with best race distance in Thoroughbreds; however, its functional and genome-wide relevance were uncertain. Additional re-sequencing in the flanking regions of the MSTN gene revealed four novel 3' UTR SNPs and a 227 bp SINE insertion polymorphism in the 5' UTR promoter sequence. Linkage disequilibrium was highest between g.66493737C>T and BIEC2-417495 (r² = 0.86).
Comparative association tests consistently demonstrated the g.66493737C>T SNP as the superior variant in the prediction of distance aptitude in racehorses (g.66493737C>T, P = 1.02 x 10⁻¹⁰; BIEC2-417495, P(unadj.) = 1.61 x 10⁻⁹). Functional investigations will be required to determine whether this polymorphism affects putative transcription-factor binding and gives rise to variation in gene and protein expression. Nonetheless, this study demonstrates that the g.66493737C>T SNP provides the most powerful genetic marker for prediction of race distance aptitude in Thoroughbreds.
几个世纪以来,人们一直致力于挑选具有速度和耐力特质的纯血马。人们普遍认识到,个体在比赛距离方面的适应性差异是由遗传变异引起的,而肌肉表型尤为重要。
使用 EquineSNP50 Bead Chip 基因分型芯片,对 118 匹具有不同比赛距离适应性的精英纯血赛马进行了最佳比赛距离的全基因组 SNP 关联研究。在基于队列的关联测试中,我们评估了适合短距离(≤ 8 弗隆)和中长距离(> 8 弗隆)比赛的马匹之间 40977 个 SNP 的基因型变异。最显著的 SNP 位于 18 号染色体上:BIEC2-417495 距离编码肌肉生长抑制素(MSTN)的基因约 690 kb[未调整 P 值(P(unadj.))= 6.96 x 10⁻⁶]。考虑到最佳比赛距离是一种定量表型,在包含 1.7 Mb 区域的 8 个 SNP 的染色体 18 上观察到一个关联峰(chr18:65809482-67545806)。同样,类似于基于队列的分析,最显著的 SNP 是 BIEC2-417495(未调整 P 值(P(unadj.))= 1.61 x 10⁻⁹;Bonferroni 调整 P 值(P(Bonf.))= 6.58 x 10⁻⁵)。在我们之前报道的候选基因研究中,MSTN 中的一个 SNP(g.66493737C>T)与纯血马的最佳比赛距离有关;然而,其功能和全基因组相关性尚不确定。在 MSTN 基因侧翼区域的进一步测序揭示了四个新的 3'UTR SNP 和 5'UTR 启动子序列中的一个 227 bp SINE 插入多态性。g.66493737C>T 和 BIEC2-417495 之间的连锁不平衡最高(r²=0.86)。
比较关联测试一致表明,g.66493737C>T SNP 是预测赛马比赛距离适应性的最佳变体(g.66493737C>T,P=1.02 x 10⁻¹⁰;BIEC2-417495,P(unadj.)=1.61 x 10⁻⁹)。需要进行功能研究以确定该多态性是否影响假定的转录因子结合并导致基因和蛋白质表达的变化。尽管如此,本研究表明,g.66493737C>T SNP 是预测纯血马比赛距离适应性的最有力遗传标记。
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