首页> 外文OA文献 >\u3cem\u3eCOL9A2\u3c/em\u3e and \u3cem\u3eCOL9A3\u3c/em\u3e Mutations in Canine Autosomal Recessive Oculoskeletal Dysplasia
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\u3cem\u3eCOL9A2\u3c/em\u3e and \u3cem\u3eCOL9A3\u3c/em\u3e Mutations in Canine Autosomal Recessive Oculoskeletal Dysplasia

机译:\ u3cem \ u3eCOL9A2 \ u3c / em \ u3e和\ u3cem \ u3eCOL9A3 \ u3c / em \ u3e犬常染色体隐性遗传性眼球骨骼发育不良的突变

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摘要

Oculoskeletal dysplasia segregates as an autosomal recessive trait in the Labrador retriever and Samoyed canine breeds, in which the causative loci have been termed drd1 and drd2, respectively. Affected dogs exhibit short-limbed dwarfism and severe ocular defects. The disease phenotype resembles human hereditary arthro-ophthalmopathies such as Stickler and Marshall syndromes, although these disorders are usually dominant. Linkage studies mapped drd1 to canine chromosome 24 and drd2 to canine chromosome 15. Positional candidate gene analysis then led to the identification of a 1-base insertional mutation in exon 1 of COL9A3 that cosegregates with drd1 and a 1,267-bp deletion mutation in the 5′ end of COL9A2 that cosegregates with drd2. Both mutations affect the COL3 domain of the respective gene. Northern analysis showed that RNA expression of the respective genes was reduced in affected retinas. These models offer potential for studies such as protein-protein interactions between different members of the collagen gene family, regulation and expression of these genes in retina and cartilage, and even opportunities for gene therapy.
机译:在拉布拉多犬和萨摩犬犬种中,眼骨骼发育异常是常染色体隐性遗传,其中致病基因座分别称为drd1和drd2。患病的狗表现出短肢侏儒症和严重的眼缺陷。该疾病的表型类似于人类遗传性眼-眼病,例如Stickler和Marshall综合征,尽管这些疾病通常占主导地位。连锁研究将drd1映射到犬24号染色体,将drd2映射到犬15号染色体。然后,通过定位候选基因分析,确定了COL9A3外显子1中的1个碱基插入突变,该突变与drd1和5个中的1,267bp缺失突变共同分离。与drd2共聚的COL9A2'末端。两种突变均影响各自基因的COL3结构域。 Northern分析显示,在受影响的视网膜中各个基因的RNA表达降低。这些模型提供了研究潜力,例如胶原蛋白基因家族不同成员之间的蛋白质-蛋白质相互作用,这些基因在视网膜和软骨中的调控和表达,甚至是基因治疗的机会。

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