Abstract

BackgroundIncubation 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.ResultsThe 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.ConclusionsWe 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.

Highlights

  • Incubation period, disease progression, pathology and clinical presentation of classical scrapie in sheep are highly dependent on Prion protein gene (PRNP) genotype, time and route of inoculation and prion strain

  • Animals Animals in the control group remained healthy without any clinical symptoms for the full experimental period

  • No obvious clinical signs of illness were visible in the scrapie group until 22 wpi, subtle signs of unspecific ill-thrift were observed in two animals from 19 wpi

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Summary

Introduction

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. The PrP genotype influences the degree of susceptibility, and the course of Meling et al BMC Veterinary Research (2018) 14:281 disease, incubation period and clinical picture [7, 11]. This genetic susceptibility is the basis behind the breeding for resistance program successfully implemented in the EU as per EC Regulation 999/2001, where only ewes carrying at least one ARR allele and no VRQ allele, and rams of ARR/ARR genotype, are bred from [12]. The prevalence of classical scrapie at population level decreased as highly susceptible genotypes are eliminated

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