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Genome-wide association analysis of canine atopic dermatitis and identification of disease related SNPs

机译:犬特应性皮炎的全基因组关联分析和疾病相关SNP的鉴定

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In humans, genome-wide association studies (GWAS) have been shown to be an effective and thorough approach for identifying polymorphisms associated with disease phenotypes. Here, we describe the first study to perform a genome-wide association study in canine atopic dermatitis (cAD) using the Illumina Canine SNP20 array, containing 22,362 single-nucleotide polymorphisms (SNPs). The aim of the study was to identify SNPs associated with cAD using affected and unaffected Golden Retrievers. Further validation studies were performed for potentially associated SNPs using Sequenom genotyping of larger numbers of cases and controls across eight breeds (Boxer, German Shepherd Dog, Labrador, Golden Retriever, Shiba Inu, Shih Tzu, Pit Bull, and West Highland White Terriers). Using meta-analysis, two SNPs were associated with cAD in all breeds tested. RS22114085 was identified as a susceptibility locus (p?=?0.00014, odds ratio?=?2) and RS23472497 as a protective locus (p?=?0.0015, odds ratio?=?0.6). Both of these SNPs were located in intergenic regions, and their effects have been demonstrated to be independent of each other, highlighting that further fine mapping and resequencing is required of these areas. Further, 12 SNPs were validated by Sequenom genotyping as associated with cAD, but these were not associated with all breeds. This study suggests that GWAS will be a useful approach for identifying genetic risk factors for cAD. Given the clinical heterogeneity within this condition and the likelihood that the relative genetic effect sizes are small, greater sample sizes and further studies will be required.
机译:在人类中,全基因组关联研究(GWAS)已被证明是识别与疾病表型相关的多态性的有效且彻底的方法。在这里,我们描述了第一个使用Illumina犬SNP20阵列在犬特应性皮炎(cAD)中进行全基因组关联研究的研究,该阵列包含22,362个单核苷酸多态性(SNP)。该研究的目的是使用受影响和未受影响的金毛猎犬鉴定与cAD相关的SNP。使用Sequenom对8个品种(拳击手,德国牧羊犬,拉布拉多,金毛猎犬,柴犬,西施,斗牛犬和西高地白梗)的大量病例和对照进行基因分型,对潜在关联的SNP进行了进一步的验证研究。使用荟萃分析,在所有测试品种中,两个SNP与cAD相关。 RS22114085被确定为敏感性位点(p≥0.00014,比值比= 2),而RS23472497被确定为保护位点(p = 0.0015,比值比= 0.6)。这两个SNP均位于基因间区域,并且其作用已被证明彼此独立,突显了这些区域还需要进一步的精细作图和重新测序。此外,通过Sequenom基因分型验证了12个SNP与cAD相关,但并不与所有品种相关。这项研究表明,GWAS将是识别cAD遗传危险因素的有用方法。考虑到这种情况下的临床异质性以及相对遗传效应量较小的可能性,将需要更大的样本量和进一步的研究。

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