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扩展犬白细胞抗原 (DLA) 单核苷酸多态性 (SNP) 基因分型揭示了虚假的 II 类关联。

Expanded dog leukocyte antigen (DLA) single nucleotide polymorphism (SNP) genotyping reveals spurious class II associations.

机构信息

School of Veterinary Medicine, University of California, Davis, USA.

出版信息

Vet J. 2011 Aug;189(2):220-6. doi: 10.1016/j.tvjl.2011.06.023. Epub 2011 Jul 7.

Abstract

The dog leukocyte antigen (DLA) system contains many of the functional genes of the immune system, thereby making it a candidate region for involvement in immune-mediated disorders. A number of studies have identified associations between specific DLA class II haplotypes and canine immune hemolytic anemia, thyroiditis, immune polyarthritis, type I diabetes mellitus, hypoadrenocorticism, systemic lupus erythematosus-related disease complex, necrotizing meningoencephalitis (NME) and anal furunculosis. These studies have relied on sequencing approximately 300 bases of exon 2 of each of the DLA class II genes: DLA-DRB1, DLA-DQA1 and DLA-DQB1. In the present study, an association (odds ratio=4.29) was identified by this method between Weimaraner dogs with hypertrophic osteodystrophy (HOD) and DLA-DRB1∗01501. To fine map the association with HOD, a genotyping assay of 126 coding single nucleotide polymorphisms (SNPs) from across the entire DLA, spanning a region of 2.5 Mb (3,320,000-5,830,000) on CFA12, was developed and tested on Weimaraners with HOD, as well as two additional breeds with diseases associated with DLA class II: Nova Scotia duck tolling retrievers with hypoadrenocorticism and Pug dogs with NME. No significant associations were found between Weimaraners with HOD or Nova Scotia duck tolling retrievers with hypoadrenocorticism and SNPs spanning the DLA region. In contrast, significant associations were found with NME in Pug dogs, although the associated region extended beyond the class II genes. By including a larger number of genes from a larger genomic region, a SNP genotyping assay was generated that provides coverage of the extended DLA region and may be useful in identifying and fine mapping DLA associations in dogs.

摘要

犬白细胞抗原 (DLA) 系统包含许多免疫系统的功能基因,因此成为免疫介导疾病相关的候选区域。许多研究已经确定了特定 DLA Ⅱ类单倍型与犬免疫性溶血性贫血、甲状腺炎、免疫性多关节炎、Ⅰ型糖尿病、肾上腺皮质功能减退症、系统性红斑狼疮相关疾病复合征、坏死性脑膜脑炎(NME)和肛门疖病之间的关联。这些研究依赖于对每个 DLA Ⅱ类基因的外显子 2 约 300 个碱基进行测序:DLA-DRB1、DLA-DQA1 和 DLA-DQB1。在本研究中,通过这种方法在患有肥大性骨营养不良症(HOD)的威玛犬中发现了与 DLA-DRB1∗01501 的关联(优势比=4.29)。为了精细定位与 HOD 的关联,开发了一种跨越整个 DLA 的 126 个编码单核苷酸多态性(SNP)的基因分型检测方法,该方法跨越 CFA12 上的 2.5 Mb 区域(3,320,000-5,830,000),并在患有 HOD 的威玛犬以及另外两种与 DLA Ⅱ类相关疾病的品种:患有肾上腺皮质功能减退症的新斯科舍诱鸭寻猎犬和患有 NME 的哈巴狗中进行了测试。在患有 HOD 的威玛犬或患有肾上腺皮质功能减退症的新斯科舍诱鸭寻猎犬中,未发现与跨越 DLA 区域的 SNP 之间存在显著关联。相反,在患有 NME 的哈巴狗中发现了与 SNP 的显著关联,尽管相关区域超出了Ⅱ类基因。通过包括来自更大基因组区域的更多基因,生成了 SNP 基因分型检测方法,该方法提供了扩展的 DLA 区域的覆盖范围,并且可能有助于鉴定和精细定位犬类中的 DLA 关联。

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