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BSE

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Title: BSE

1

BSE
MAD COW DISEASE
2005

Anette Rink, DVM, PhD
Animal Disease and Food Safety Laboratory
Nevada Department of Agriculture
350 Capitol Hill Avenue
Reno NV 89502

2
Prions

Proteinaceous infectious particle
Composed only of protein
no nucleic acid (DNA or RNA)
Multiple strains
Present in non-infected and infected cells
Host-coded normal cellular protein that becomes
partially protease-resistant through
post-translational conformation change

abnormal folding
PrPC
PrPBSE/Sc
Host genetics PrPBSE/Sc
Normal form
BSE form
3
Prions, cont.

Pathologically characterized by the triad
Spongiform change
Neuronal loss
Reactive gliosis
PrPSc has the ability to convert normal prions
into its own aberrant structure by a
template-directed folding mechanism
PrPSc is non-functional and may deplete the
brain of the physiological function of PrPC

4
Role of PrPC in Copper Homeostasis

Located at the pre-synaptic membrane
Most abundant in the CNS but expressed in most
non-neuronal tissues
Predominantly pre-synaptic function in synaptic
transmission and neuronal excitability
Cu(II) binding at N-terminal octapeptide
Highly conserved domain amongst species
Acts as a buffer for Cu(II) in the synaptic cleft

5
Neuroprotective Properties of PrPC

Neuroprotective molecule, response to
pro-oxidative insults
Lack of PrPC results in neuronal phenotypes
sensitive to oxidative stress induced by
superoxide (O2.-) and H2O2
PrPC inhibits BAX induced apoptosis in vitro

6
Involvement of PrPC in neuronal Ca2 Disturbances

Loss of normal prion protein is associated with
disturbance in neuronal calcium homeostasis
Influences mechanisms of Ca2 release from
internal ER
Ca2 is a critical component of signaling
pathways leading to structural and functional
neuronal changes
Modulator of Ca2 flux in response to Cu(II) or
SOD activity enabling of redox signaling an
metal dependent biochemical and cellular
processes

7
Schematic representatin of the physiological role
of prion protein (PrPC) in copper homeostasis and
redox signalling.
8
Transmissible Spongiform Encephalopathies (TSEs)

Long incubation period (2-8 years for BSE)
Progressively debilitating neurological illnesses
Pathologic changes are confined to the CNS
Presence of Scrapie-Associated Fibrils (EM)
Elicit no detectable immune response
Always fatal

9
TSE Agent Theories

VIRUS
Unusual biochemical biophysical characteristics
No nucleic acid identified
No particle found under electron microscopy
VIRINO
Host-derived protein coat (PrP?) small
non-coding regulatory nucleic acid
No nucleic acid identified
No particle found under electron microscopy
PRION
Host-coded normal cellular protein that becomes
partially protease resistant through
post-translational conformation change
Most widely accepted theory

10
TSEs - Humans

Creutzfeldt-Jakob Disease (CJD)
Gerstmann-Straussler-Scheinker Syndrome (GSS)
Fatal Familial Insomnia (FFI)
Kuru
Variant Creutzfeldt-Jakob Disease (vCJD)

11
TSEs - Other Animals

Scrapie
Sheep and goats
Known for 250 years
Chronic Wasting Disease (CWD)
Captive elk free-ranging deer and elk
First recognized in deer in 1967
Transmissible Mink Encephalopathy (TME)
Mink
First recognized in mink in 1947
Feline Spongiform Encephalopathy (FSE)
Cats
First recognized in 1990
Associated with BSE

12
BOVINE SPONGIFORM ENCEPHALOPATHY
13
Bovine Spongiform Encephalopathy

Bovine Spongiform Encephalopathy (BSE), commonly
known as Mad Cow Disease, is a chronic
degenerative disease affecting the central
nervous system of cattle and which has been
linked to a similar disease in humans, variant
Creutzfedlt-Jakob Disease.

14
Origin of BSE

First case was identified in 1986
Epidemiologic evidence
Common source
Feed containing TSE-contaminated meat and bone
meal
sheep with scrapie?
rendering changes in the 1980s?
discontinuance of solvent extraction (steam-heat
treatment)
amplification
cattle with previously unidentified TSE?
cattle were first probably infected in the 1970s
there are some 35 theories as to the origin of
BSE in UK cattle

15
Clinical Signs

Incubation (2 to 8 years)
Gradual deterioration
Recumbency, death, destruction
2 weeks to 6 months
Neurologic symptoms
Apprehension, fear, increased startle, or
depression
Hyperaesthesia or hyperreflexia
Muscle fasciculations, tremors, and myoclonus
Ataxia (incoordination, hypermetria)
Autonomic dysfunction
reduced rumination, bradycardia and altered heart
rhythm
Progressive weight loss

16
Differential Diagnosis

Rabies
Milk fever
Lead poisoning (or other toxin)
Grass tetany
Nervous ketosis
Listeriosis
Encephalitis
Thiamine deficiency
Brain tumor

17
Tissue Infectivity
Brain Trigeminal ganglia
Spinal cord Dorsal root ganglia
Retina
Bone marrow
Distal ileum (Small intestine)

Natural infection
Experimental infection

NOTE Distribution may involve lymphoreticular
tissues in other species.
18
BSE in Great Britain
Total through 2002 183,191 cases
19
Italy Japan Israel Finland Slovakia Slovenia Greec
e Austria Czech Republic
First cases of BSE
Liechtenstein
Great Britain
Portugal Switzerland
Denmark Germany Spain
Netherlands Belgium Luxembourg
Canada U. S. ()
France
Ireland
98
90
94
2003
1986
Imported from Canada
20

BSE Incidence Rate (per million cattle gt 2 yrs)

98
99 02 United Kingdom
677 482 248 Portugal
159 199 108 Switzerland 16
59 28 Ireland
21 22 88 France
2 3 21 Belgium
4 2
26 Netherlands 1
1 13
21
vCJD Cases(as of 11/3/2003)152 cases
vCJD cases 137 (plus 6 probable)
1 (imported)
vCJD cases - 6
1 (imported)