首页> 美国卫生研究院文献>Veterinary Research >Bovine Neonatal Pancytopenia is a heritable trait of the dam rather than the calf and correlates with the magnitude of vaccine induced maternal alloantibodies not the MHC haplotype
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Bovine Neonatal Pancytopenia is a heritable trait of the dam rather than the calf and correlates with the magnitude of vaccine induced maternal alloantibodies not the MHC haplotype

机译:牛新生儿全血细胞减少症是大坝而不是小腿的可遗传特征并且与疫苗诱导的母源同种抗体的大小有关而不与MHC单倍型有关

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摘要

Bovine Neonatal Pancytopenia (BNP), a bleeding syndrome of neonatal calves, is caused by alloantibodies absorbed from the colostrum of particular cows. A commercial BVD vaccine is the likely source of alloantigens eliciting BNP associated alloantibodies. We hypothesized that the rare occurrence of BNP in calves born to vaccinated dams could be associated with genetic differences within dams and calves. We found that the development of BNP within calves was a heritable trait for dams, not for calves and had a high heritability of 19%. To elucidate which genes play a role in the development of BNP we sequenced candidate genes and characterized BNP alloantibodies. Alloantigens present in the vaccine have to be presented to the dam’s immune system via MHC class II, however sequencing of DRB3 showed no differences in MHC class II haplotype between BNP and non-BNP dams. MHC class I, a highly polymorphic alloantigen, is an important target of BNP alloantibodies. Using a novel sequence based MHC class I typing method, we found no association of BNP with MHC class I haplotype distribution in dams or calves. Alloantibodies were detected in both vaccinated BNP and non-BNP dams and we found no differences in alloantibody characteristics between these groups, but alloantibody levels were significantly higher in BNP dams. We concluded that the development of BNP in calves is a heritable trait of the dam rather than the calf and genetic differences between BNP and non-BNP dams are likely due to genes controlling the quantitative alloantibody response following vaccination.Electronic supplementary materialThe online version of this article (doi:10.1186/s13567-014-0129-0) contains supplementary material, which is available to authorized users.
机译:牛新生全血细胞减少症(BNP)是一种新生牛犊的出血综合征,是由从特定母牛的初乳吸收的同种抗体引起的。商业化的BVD疫苗可能是引起BNP相关同种抗体的同种抗原的来源。我们假设,在接种大坝的小牛中,BNP的罕见发生可​​能与大坝和小牛内的遗传差异有关。我们发现,小牛体内BNP的发育是水坝的遗传特征,而不是小牛,遗传力高达19%。为了阐明哪些基因在BNP的发育中起作用,我们对候选基因进行了测序并表征了BNP同种抗体。疫苗中存在的同种抗原必须通过II类MHC提交大坝的免疫系统,但是DRB3的测序表明BNP和非BNP大坝在II类MHC单倍型上没有差异。 MHC I类是高度多态的同种抗原,是BNP同种抗体的重要靶标。使用基于序列的新型MHC I类分型方法,我们发现在大坝或小牛中BNP与MHC I类单倍型分布没有关联。在接种的BNP和非BNP母犬中均检测到同种抗体,我们发现这些组之间的同种抗体特征没有差异,但BNP母鼠中的同种抗体水平明显更高。我们得出的结论是,小牛体内BNP的发育是小牛的遗传特征,而不是小牛,BNP和非BNP大坝之间的遗传差异很可能是由于基因控制了疫苗接种后异源抗体的定量反应。文章(doi:10.1186 / s13567-014-0129-0)包含补充材料,授权用户可以使用。

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