Julia H Segert, Jana-Marie Seidel, Walter J Wurzer, Anja M Geretschlaeger
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Furthermore, establish a possible link between bleeding phenotype, vWF serum concentrations and <i>VWF</i> mutation status.</p><p><strong>Results: </strong>Eighty-seven Kromfohrländer were genotyped for the G > A von Willebrand type I mutation. For detection of the associated mutation we used an endpoint genotyping method. We identified the G > A von Willebrand type I mutation in 80.5% of our study population. 65.5% were heterozygous (WT/MUT) and 15.0% were homozygous for the mutation (MUT/MUT). 21% of the overall study population exhibited bleeding symptoms. 45.5% of all homozygous dogs (MUT/MUT) showed bleeding symptoms. In contrast, wild-type homozygotes exhibited no bleeding symptoms, whereas 23.2% of the heterozygotes did. VWF serum concentrations varied from 28 to 137% in wild-type dogs while in heterozygous and homozygous dogs the concentration ranged from 3 to 77% and 1 to 23%, respectively (<i>p</i> < 0.05).</p><p><strong>Conclusion: </strong>Based on our data, we found the G > A mutation in the <i>VWF</i> gene in the Kromfohrländer breed and the subsequent vWDI as the underlying cause for the bleeding episodes and delayed coagulation in heterozygous and homozygous dogs. Since both, heterozygotes and homozygotes show reduced vWF serum concentrations and exhibit to a certain percentage the vWD syndrome phenotype, we postulate that, in contrast to most other vWDI affected breeds, inheritance follows an autosomal dominant mode with incomplete penetrance.</p>","PeriodicalId":91060,"journal":{"name":"Canine genetics and epidemiology","volume":"6 ","pages":"3"},"PeriodicalIF":0.0000,"publicationDate":"2019-05-16","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://sci-hub-pdf.com/10.1186/s40575-019-0073-4","citationCount":"3","resultStr":"{\"title\":\"vWDI is inherited in an autosomal dominant manner with incomplete penetrance, in the Kromfohrländer breed.\",\"authors\":\"Julia H Segert, Jana-Marie Seidel, Walter J Wurzer, Anja M Geretschlaeger\",\"doi\":\"10.1186/s40575-019-0073-4\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Background: </strong>Von Willebrand disorder type I (vWDI) is known as an inherited bleeding disorder in different dog breeds following an autosomal recessive inheritance. The Kromfohrländer is a rare dog breed with an increased incidence of unclear bleeding episodes and prolonged coagulation time during/after surgery or injuries, indicating a defect in one or more critical proteins of the coagulation cascade.</p><p><strong>Objective: </strong>The objective of this study was to determine whether the c.7437G > A mutation in the <i>VWF</i> gene previously shown to cause von Willebrand disorder type I in Doberman Pinscher is also linked to this disease in the Kromfohrländer breed and to serum concentrations of vWF. Furthermore, establish a possible link between bleeding phenotype, vWF serum concentrations and <i>VWF</i> mutation status.</p><p><strong>Results: </strong>Eighty-seven Kromfohrländer were genotyped for the G > A von Willebrand type I mutation. For detection of the associated mutation we used an endpoint genotyping method. We identified the G > A von Willebrand type I mutation in 80.5% of our study population. 65.5% were heterozygous (WT/MUT) and 15.0% were homozygous for the mutation (MUT/MUT). 21% of the overall study population exhibited bleeding symptoms. 45.5% of all homozygous dogs (MUT/MUT) showed bleeding symptoms. In contrast, wild-type homozygotes exhibited no bleeding symptoms, whereas 23.2% of the heterozygotes did. VWF serum concentrations varied from 28 to 137% in wild-type dogs while in heterozygous and homozygous dogs the concentration ranged from 3 to 77% and 1 to 23%, respectively (<i>p</i> < 0.05).</p><p><strong>Conclusion: </strong>Based on our data, we found the G > A mutation in the <i>VWF</i> gene in the Kromfohrländer breed and the subsequent vWDI as the underlying cause for the bleeding episodes and delayed coagulation in heterozygous and homozygous dogs. 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引用次数: 3
摘要
背景:血管性血友病I型(vWDI)是一种常染色体隐性遗传的不同犬种的遗传性出血性疾病。Kromfohrländer是一种罕见的犬种,在手术或受伤期间/之后,不清楚出血发作的发生率增加,凝血时间延长,表明凝血级联的一种或多种关键蛋白存在缺陷。目的:本研究的目的是确定先前在杜宾平切犬中引起血管性血液病I型的VWF基因的c.7437G > A突变是否也与Kromfohrländer品种的这种疾病和VWF的血清浓度有关。此外,建立出血表型、vWF血清浓度和vWF突变状态之间的可能联系。结果:87例Kromfohrländer基因分型为G > A von Willebrand I型突变。为了检测相关突变,我们使用了终点基因分型方法。我们在80.5%的研究人群中发现了G > A von Willebrand I型突变。65.5%为杂合子(WT/MUT), 15.0%为纯合子(MUT/MUT)。21%的研究人群出现出血症状。45.5%的纯合子犬(MUT/MUT)出现出血症状。相比之下,野生型纯合子没有出血症状,而23.2%的杂合子有出血症状。野生型犬血清VWF浓度为28 ~ 137%,杂合型和纯合型犬血清VWF浓度分别为3 ~ 77%和1 ~ 23% (p)结论:根据我们的数据,我们发现Kromfohrländer品种VWF基因G > A突变和随后的vWDI是导致杂合型和纯合型犬出血和凝血延迟的根本原因。由于杂合子和纯合子均表现出vWF血清浓度降低,并在一定比例上表现出vWD综合征表型,因此我们假设,与大多数其他vWDI影响品种相比,遗传遵循常染色体显性模式,具有不完全外显率。
vWDI is inherited in an autosomal dominant manner with incomplete penetrance, in the Kromfohrländer breed.
Background: Von Willebrand disorder type I (vWDI) is known as an inherited bleeding disorder in different dog breeds following an autosomal recessive inheritance. The Kromfohrländer is a rare dog breed with an increased incidence of unclear bleeding episodes and prolonged coagulation time during/after surgery or injuries, indicating a defect in one or more critical proteins of the coagulation cascade.
Objective: The objective of this study was to determine whether the c.7437G > A mutation in the VWF gene previously shown to cause von Willebrand disorder type I in Doberman Pinscher is also linked to this disease in the Kromfohrländer breed and to serum concentrations of vWF. Furthermore, establish a possible link between bleeding phenotype, vWF serum concentrations and VWF mutation status.
Results: Eighty-seven Kromfohrländer were genotyped for the G > A von Willebrand type I mutation. For detection of the associated mutation we used an endpoint genotyping method. We identified the G > A von Willebrand type I mutation in 80.5% of our study population. 65.5% were heterozygous (WT/MUT) and 15.0% were homozygous for the mutation (MUT/MUT). 21% of the overall study population exhibited bleeding symptoms. 45.5% of all homozygous dogs (MUT/MUT) showed bleeding symptoms. In contrast, wild-type homozygotes exhibited no bleeding symptoms, whereas 23.2% of the heterozygotes did. VWF serum concentrations varied from 28 to 137% in wild-type dogs while in heterozygous and homozygous dogs the concentration ranged from 3 to 77% and 1 to 23%, respectively (p < 0.05).
Conclusion: Based on our data, we found the G > A mutation in the VWF gene in the Kromfohrländer breed and the subsequent vWDI as the underlying cause for the bleeding episodes and delayed coagulation in heterozygous and homozygous dogs. Since both, heterozygotes and homozygotes show reduced vWF serum concentrations and exhibit to a certain percentage the vWD syndrome phenotype, we postulate that, in contrast to most other vWDI affected breeds, inheritance follows an autosomal dominant mode with incomplete penetrance.
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