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斯卢夫猎犬的全身性进行性视网膜萎缩是由PDE6B基因第21外显子中的一个8碱基对插入所致。

Generalized progressive retinal atrophy of Sloughi dogs is due to an 8-bp insertion in exon 21 of the PDE6B gene.

作者信息

Dekomien G, Runte M, Gödde R, Epplen J T

机构信息

Molecular Human Genetics, Ruhr-University, Bochum, Germany.

出版信息

Cytogenet Cell Genet. 2000;90(3-4):261-7. doi: 10.1159/000056785.

Abstract

We investigated the gene encoding the beta subunit of cGMP phosphodiesterase (PDE6B) as a candidate for generalized progressive retinal atrophy (gPRA), an autosomal recessively transmitted eye disease in dogs. The PDE6B gene was isolated from a genomic library. Single-strand conformation polymorphism analysis revealed eight intronic variations in different subsets of the 14 dog breeds investigated. In addition, we identified an 8-bp insertion after codon 816 in certain Sloughi dogs. Analysis of PRA-affected and obligatory carrier Sloughis showed that this mutation cosegregates with disease status in a large pedigree. All other exchanges identified were not located in functionally relevant parts of the gene (e.g., in the splice signal consensus sites). In most dog breeds (Labrador retriever, Tibetan mastiff, dachshund, Tibetan terrier, miniature poodle, Australian cattle dog, cocker spaniel, collie, Saarloos wolfhound, Chesapeake Bay retriever, and Yorkshire terrier), PDE6B was excluded as a candidate gene for gPRA because heterozygous allele constellations were detected in diseased animals. Therefore, the PDE6B sequence variations did not segregate together with the mutation(s) causing gPRA. Direct and indirect DNA tests concerning gPRA can be offered now for a variety of different dog breeds.

摘要

我们研究了编码环磷酸鸟苷磷酸二酯酶(PDE6B)β亚基的基因,将其作为犬类常染色体隐性遗传眼病——全身性进行性视网膜萎缩(gPRA)的候选基因。从基因组文库中分离出PDE6B基因。单链构象多态性分析揭示了在所研究的14个犬种的不同亚组中有8个内含子变异。此外,我们在某些斯卢夫猎犬中鉴定出第816密码子后有一个8碱基对的插入。对受PRA影响的和必然携带该基因的斯卢夫猎犬进行分析表明,在一个大型家系中,这种突变与疾病状态共分离。鉴定出的所有其他交换都不在该基因的功能相关部分(例如,不在剪接信号共有位点)。在大多数犬种(拉布拉多寻回犬、藏獒、腊肠犬、西藏梗犬、迷你贵宾犬、澳大利亚牧牛犬、可卡犬、柯利牧羊犬、萨阿路斯狼猎犬、切萨皮克湾寻回犬和约克夏梗犬)中,PDE6B被排除作为gPRA的候选基因,因为在患病动物中检测到杂合等位基因组合。因此,PDE6B序列变异并未与导致gPRA的突变一起分离。现在可以针对多种不同犬种提供有关gPRA的直接和间接DNA检测。

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