首页> 外文期刊>BMC Veterinary Research >Expression of selected genes isolated from whole blood, liver and obex in lambs with experimental classical scrapie and healthy controls, showing a systemic innate immune response at the clinical end-stage
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Expression of selected genes isolated from whole blood, liver and obex in lambs with experimental classical scrapie and healthy controls, showing a systemic innate immune response at the clinical end-stage

机译:在实验性经典瘙痒病和健康对照组中,从全血,肝和肥胖中分离出的选定基因的表达,在临床后期显示出系统性先天免疫反应

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Incubation period, disease progression, pathology and clinical presentation of classical scrapie in sheep are highly dependent on PRNP genotype, time and route of inoculation and prion strain. Our experimental model with pre-colostrum inoculation of homozygous VRQ lambs has shown to be an effective model with extensive PrPSc dissemination in lymphatic tissue and a short incubation period with severe clinical disease. Serum protein analysis has shown an elevation of acute phase proteins in the clinical stages of this experimental model, and here, we investigate changes in gene expression in whole blood, liver and brain. The animals in the scrapie group showed severe signs of illness 22?weeks post inoculation necessitating euthanasia at 23?weeks post inoculation. This severe clinical presentation was accompanied by changes in expression of several genes. The following genes were differentially expressed in whole blood: TLR2, TLR4, C3, IL1B, LF and SAA, in liver tissue, the following genes differentially expressed: TNF-α, SAA, HP, CP, AAT, TTR and TF, and in the brain tissue, the following genes were differentially expressed: HP, CP, ALB and TTR. We report a strong and evident transcriptional innate immune response in the terminal stage of classical scrapie in these animals. The PRNP genotype and time of inoculation are believed to contribute to the clinical presentation, including the extensive dissemination of PrPSc throughout the lymphatic tissue.
机译:绵羊经典瘙痒病的潜伏期,疾病进展,病理学和临床表现高度依赖于PRNP基因型,接种时间和途径以及病毒株。我们的初乳前接种纯合VRQ羔羊的实验模型显示,它是一种有效的模型,在淋巴组织中具有广泛的PrPSc传播,并且具有严重的临床疾病,潜伏期短。血清蛋白分析显示该实验模型在临床阶段急性期蛋白水平升高,在这里,我们研究了全血,肝和脑中基因表达的变化。瘙痒病组中的动物在接种后22周出现严重疾病迹象,因此必须在接种后23周实施安乐死。这种严重的临床表现伴随着几种基因表达的变化。以下基因在全血中差异表达:TLR2,TLR4,C3,IL1B,LF和SAA,在肝组织中,以下基因差异表达:TNF-α,SAA,HP,CP,AAT,TTR和TF,以及在脑组织中,以下基因被差异表达:HP,CP,ALB和TTR。我们报告了在这些动物的经典瘙痒病的终结阶段的强大和明显的转录先天免疫反应。据信PRNP基因型和接种时间有助于临床表现,包括PrPSc在整个淋巴组织中的广泛传播。

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