Experimental Classical Bovine Spongiform Encephalopathy

Author:

Simmons M. M.12,Spiropoulos J.12,Webb P. R.1,Spencer Y. I.1,Czub S.34,Mueller R.5,Davis A.16,Arnold M. E.7,Marsh S.1,Hawkins S. A. C.1,Cooper J. A.1,Konold T.1,Wells G. A. H.1

Affiliation:

1. Department of Pathology, Veterinary Laboratories Agency, Addlestone, Surrey, UK

2. These authors have contributed equally to this work.

3. Canadian Food Inspection Agency, Winnipeg Laboratory, Winnipeg, Manitoba, R3E 3M4, Canada

4. Present affiliation: Canadian Food Inspection Agency, Lethbridge Laboratory, Lethbridge, Alberta, Canada

5. Health Canada, Health Products and Food Branch, Tunney’s Pasture, Ottawa, Ontario, Canada

6. Present affiliation: Dorevitch Pathology, Coburg, Victoria, Australia

7. Centre for Epidemiology and Risk Analysis, VLA Sutton Bonington, Sutton Bonington, Loughborough, Leicestershire, UK

Abstract

Tissues from sequential-kill time course studies of bovine spongiform encephalopathy (BSE) were examined to define PrP immunohistochemical labeling forms and map disease-specific labeling over the disease course after oral exposure to the BSE agent at two dose levels. Study was confined to brainstem, spinal cord, and certain peripheral nervous system ganglia—tissues implicated in pathogenesis and diagnosis or disease control strategies. Disease-specific labeling in the brainstem in 39 of 220 test animals showed the forms and patterns observed in natural disease and invariably preceded spongiform changes. A precise temporal pattern of increase in labeling was not apparent, but labeling was generally most widespread in clinical cases, and it always involved neuroanatomic locations in the medulla oblongata. In two cases, sparse labeling was confined to one or more neuroanatomic nuclei of the medulla oblongata. When involved, the spinal cord was affected at all levels, providing no indication of temporal spread within the cord axis or relative to the brainstem. Where minimal PrP labeling occurred in the thoracic spinal cord, it was consistent with initial involvement of general visceral efferent neurons. Labeling of ganglia involved only sensory ganglia and only when PrP was present in the brainstem and spinal cord. These experimental transmissions mimicked the neuropathologic findings in BSE-C field cases, independent of dose of agent or stage of disease. The model supports current diagnostic sampling approaches and control measures for the removal and destruction of nervous system tissues in slaughtered cattle.

Publisher

SAGE Publications

Subject

General Veterinary

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