Deciphering the BSE-type specific cell and tissue tropisms of atypical (H and L) and classical BSE

Anne Balkema-Buschmann,Grit Priemer,Reiner Ulrich,Romano Strobelt,Bob Hills,Martin H Groschup

doi:10.1080/19336896.2019.1651180

Anne Balkema-Buschmann, Grit Priemer + Show 4 more

Open Access

https://doi.org/10.1080/19336896.2019.1651180

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Journal: Prion	Publication Date: Jan 1, 2019
Citations: 8	License type: open-access

Affiliation: Friedrich-Loeffler-Institut, Health Canada

Abstract

ABSTRACTAfter the discovery of two atypical bovine spongiform encephalopathy (BSE) forms in France and Italy designated H- and L-BSE, the question arose whether these new forms differed from classical BSE (C-BSE) in their pathogenesis. Samples collected from cattle in the clinical stage of BSE during an intracranial challenge study with L- and H-BSE were analysed using biochemical and histological methods as well as in a transgenic mouse bioassay. Our results generally confirmed what had been described for C-BSE to be true also for both atypical BSE forms, namely the restriction of the pathological prion protein (PrPSc) and BSE infectivity to the nervous system. However, analysis of samples collected under identical conditions from both atypical H- and L-BSE forms allowed us a more precise assessment of the grade of involvement of different tissues during the clinical end stage of disease as compared to C-BSE. One important feature is the involvement of the peripheral nervous and musculoskeletal tissues in both L-BSE and H-BSE affected cattle. We were, however, able to show that in H-BSE cases, the PrPSc depositions in the central and peripheral nervous system are dominated by a glial pattern, whereas a neuronal deposition pattern dominates in L-BSE cases, indicating differences in the cellular and topical tropism of both atypical BSE forms. As a consequence of this cell tropism, H-BSE seems to spread more rapidly from the CNS into the periphery via the glial cell system such as Schwann cells, as opposed to L-BSE which is mostly propagated via neuronal cells.

Highlights

Bovine spongiform encephalopathy (BSE) in cattle belongs to the group of transmissible spongiform encephalopathies (TSEs), called ‘prion diseases’
The optic nerve samples were detected positive for all animals sacrificed between 14 and 16 mpi, with slightly higher OD values (1.266 on average) for the samples collected from H-BSE infected cattle as compared to 0.896 on average for the L-BSE infected animals (Table 1)
PTA-WB PTA-WB of the central nervous system (CNS) samples was positive in dilutions up to 1:1024 for all 10 animals challenged with H- and L-BSE that had been in the clinical stage of the disease (Table 1)

Summary

Introduction

Bovine spongiform encephalopathy (BSE) in cattle belongs to the group of transmissible spongiform encephalopathies (TSEs), called ‘prion diseases’. These inevitably fatal neurodegenerative disorders can affect numerous mammalian species. Classical BSE (C-BSE) in cattle has been shown to be causatively linked to the feeding of BSEcontaminated meat and bone meal and milk replacers [2,3]. The prohibition of these feeding practices has effectively stopped the circulation of the BSE agent in the feed chain of bovines and drastically reduced the infection rate of cattle born after the implementation of these measures. Minor amounts of infectivity have been demonstrated in a Musc. semitendinosus sample of a natural C-BSE case in the final disease stage

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