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The three-way relationship of polymorphisms of porcine genes encoding terminal complement components, their differential expression, and health-related phenotypes

机译:编码末端补体成分的猪基因多态性的三向关系,它们的差异表达和与健康有关的表型

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Background The complement system is an evolutionary ancient mechanism that plays an essential role in innate immunity and contributes to the acquired immune response. Three modes of activation, known as classical, alternative and lectin pathway, lead to the initiation of a common terminal lytic pathway. The terminal complement components (TCCs: C6, C7, C8A, C8B, and C9) are encoded by the genes C6 , C7 , C8A , C8B , C8G , and C9 . We aimed at experimentally testing the porcine genes encoding TCCs as candidate genes for immune competence and disease resistance by addressing the three-way relationship of genotype, health related phenotype, and mRNA expression. Results Comparative sequencing of cDNAs of animals of the breeds German Landrace , Piétrain, Hampshire, Duroc, Vietnamese Potbelly Pig, and Berlin Miniature Pig (BMP) revealed 30 SNPs (21 in protein domains, 12 with AA exchange). The promoter regions (each ~1.5 kb upstream the transcription start sites) of C6 , C7 , C8A , C8G , and C9 exhibited 29 SNPs . Significant effects of the TCC encoding genes on hemolytic complement activity were shown in a cross of Duroc and BMP after vaccination against Mycoplasma hyopneumoniae, Aujeszky disease virus and PRRSV by analysis of variance using repeated measures mixed models. Family based association tests (FBAT) confirmed the associations. The promoter SNPs were associated with the relative abundance of TCC transcripts obtained by real time RT-PCR of 311 liver samples of commercial slaughter pigs. Complement gene expression showed significant relationship with the prevalence of acute and chronic lung lesions. Conclusions The analyses point to considerable variation of the porcine TCC genes and promote the genes as candidate genes for disease resistance.
机译:背景技术补体系统是一种古老的进化机制,在先天免疫中起着至关重要的作用,并有助于获得性免疫应答。三种激活方式,称为经典,替代和凝集素途径,可导致共同的末端裂解途径的启动。末端补体成分(TCC:C6,C7,C8A,C8B和C9)由基因C6,C7,C8A,C8B,C8G和C9编码。我们的目标是通过解决基因型,健康相关表型和mRNA表达的三向关系,来实验测试编码TCCs的猪基因作为免疫能力和抗病性的候选基因。结果对德国长白,皮亚特兰,汉普郡,杜洛克,越南大肚​​猪和柏林微型猪(BMP)的动物的cDNA进行比较测序,发现30个SNP(21个蛋白质域中,有12个具有AA交换)。 C6,C7,C8A,C8G和C9的启动子区域(每个在转录起始位点上游约1.5 kb)显示29个SNP。通过使用重复测量混合模型对方差进行分析,对猪肺炎支原体,Aujeszky病病毒和PRRSV接种疫苗后,杜洛克和BMP的杂交显示了TCC编码基因对溶血补体活性的显着影响。基于家庭的关联测试(FBAT)确认了关联。启动子SNP与通过实时RT-PCR获得的311只商品屠宰猪肝脏样品的TCC转录物的相对丰度相关。补体基因表达与急性和慢性肺部病变的发生率呈显着相关。结论分析表明猪TCC基因有相当大的变异,并促进了该基因成为抗病候选基因。

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