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首页> 外文期刊>Scientific reports. >Pathogenicity of Bovine Neonatal Pancytopenia-associated vaccine-induced alloantibodies correlates with Major Histocompatibility Complex class I expression
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Pathogenicity of Bovine Neonatal Pancytopenia-associated vaccine-induced alloantibodies correlates with Major Histocompatibility Complex class I expression

机译:牛新生儿全血细胞减少症相关疫苗诱导的同种抗体的致病性与主要组织相容性复合体I类表达相关

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Bovine Neonatal Pancytopenia (BNP), a fatal bleeding syndrome of neonatal calves, is caused by maternal alloantibodies absorbed from colostrum and is characterized by lymphocytopenia, thrombocytopenia and bone marrow hypoplasia. An inactivated viral vaccine is the likely source of alloantigens inducing BNP-associated alloantibodies in the dam. In this study the specificity of BNP alloantibodies was assessed and was linked to the pathology of BNP. We demonstrated that Major Histocompatibility Complex class I (MHC I) and Very Late Antigen-3, an integrin α3/β1 heterodimer, were the major targets of BNP alloantibodies. However, alloantibody binding to various bovine cell types correlated with MHC I expression, rather than integrin β1 or α3 expression. Likewise, alloantibody-dependent complement-mediated cell lysis correlated strongly with MHC I expression. Examination of several tissues of third trimester bovine foetuses revealed that cells, shown to be affected in calves with BNP, were characterized by high MHC class I expression and high levels of alloantibody binding. We conclude that in spite of the heterogeneous specificity of BNP associated maternal alloantibodies, MHC I-specific antibodies mediate the pathogenicity of BNP in the calf and that cells with high MHC I expression were preferentially affected in BNP.
机译:牛新生全血细胞减少症(BNP)是新生牛犊的致命性出血综合征,由初乳吸收的母体同种抗体引起,其特征是淋巴细胞减少,血小板减少和骨髓发育不全。灭活的病毒疫苗可能是大坝中诱导BNP相关同种抗体的同种抗原的来源。在这项研究中,评估了BNP同种抗体的特异性,并将其与BNP的病理联系在一起。我们证明了主要的组织相容性复合体I类(MHC I)和整合素α3/β1异二聚体Very Very Antigen-3是BNP同种抗体的主要靶标。然而,与各种牛细胞类型结合的同种抗体与MHC I表达相关,而不与整联蛋白β1或α3表达相关。同样,同种抗体依赖性补体介导的细胞裂解与MHC I表达密切相关。对三个月中期的牛胎儿的几个组织进行的检查显示,显示出受到BNP犊牛影响的细胞具有高I类MHC表达和高水平同种抗体结合的特征。我们得出结论,尽管BNP相关母源同种异体抗体的异质性,MHC I特异性抗体介导小牛BNP的致病性,并且具有高MHC I表达的细胞优先受到BNP的影响。

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