首页> 外文期刊>The Veterinary Journal >G244E in the canine factor IX gene leads to severe haemophilia B in Rhodesian Ridgebacks.
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G244E in the canine factor IX gene leads to severe haemophilia B in Rhodesian Ridgebacks.

机译:犬IX因子基因中的G244E在罗得西亚脊背龙中导致严重的血友病B。

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摘要

Haemophilia B in Rhodesian Ridgebacks is currently the most important canine haemophilia in Germany. The aim of this study was to define the underlying genetic defect. Genetic studies were performed including six phenotypically affected male dogs (factor IX activity: approximately 1%), four suspected carriers (factor IX activity 48-69%, one confirmed by affected offspring), and 12 healthy dogs. Comparison of the entire coding region of the canine factor IX DNA sequences and exon-intron junctions from affected dogs with the wild type canine factor IX DNA revealed a G-A missense mutation in exon 7. This mutation results in a glycine (GGA) to glutamic acid (GAA) exchange in the catalytic domain of the haemophilic factor IX. All affected dogs were hemizygous for the detected mutation and carriers were heterozygous, whereas none of the Rhodesian Ridgebacks with normal factor IX activity showed the mutation. No further alterations in the sequences between affected dogs and the healthy control group could be observed. None of the Rhodesian Ridgebacks with undefined haemophilia B status (n=30) and no individual of three other dog breeds (Doberman Pinscher: n=20; German Wire haired Pointer: n=20; Labrador: n=25) showed the presence of the mutation. Amino acid sequence alignment and protein structural modelling analysis indicate that the detected mutation causes a relevant functional defect. The results of this study suggest that the detected mutation is responsible for a severe form of haemophilia B in Rhodesian Ridgebacks
机译:罗得西亚脊背龙的B型血友病目前是德国最重要的犬血友病。这项研究的目的是确定潜在的遗传缺陷。进行了遗传研究,包括六只受表型影响的雄性狗(因子IX活性:约1%),四只可疑携带者(因子IX活性为48-69%,一只被受影响的后代确认)和12只健康的狗。将野生型犬因子IX DNA与患犬的犬因子IX DNA序列的整个编码区和外显子-内含子连接进行比较,发现外显子7中存在GA错义突变。该突变导致甘氨酸(GGA)变为谷氨酸(GAA)在嗜血因子IX的催化域中交换。所有受影响的狗的检测到的突变均为半合子,携带者为杂合子,而具有正常IX因子活性的Rhodesian Ridgebacks均未显示出该突变。在患病犬与健康对照组之间没有观察到序列的进一步改变。罗得西亚脊背龙的B型血友病状态未定义(n = 30),其他三个犬种都没有个体(Doberman Pinscher:n = 20; German Wire hair Pointer:n = 20; Labrador:n = 25)没有出现突变。氨基酸序列比对和蛋白质结构建模分析表明,检测到的突变引起相关的功能缺陷。这项研究的结果表明,检测到的突变是造成罗得西亚脊背龙严重形式的B型血友病的原因。

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