What are prions and prion diseases?
Prions are pathogenic proteins (proteinaceous infectious particle PrPsc) found in prion diseases, which are neurodegenerative diseases
What are prion diseases also known as?
Transmissible Spongiform Encephalopathy (TSEs)
Name three mammalian species where prions are found and their associated prion disease, which mammal was the first to be found with PrPscs?
- First found PrPscs in sheep with scrapie
- Mad Cow disease/ BSE
- Chronic wasting disease in deer
Name four prion diseases found in humans
- Creutzfeldt-Jakob disease (CJD) AND variant Creutzfeldt-Jakob disease (vCJD)
- Kuru
- Fatal familiar Insomnia (FFI)
- GSS
Name five symptoms of prion diseases
- Anxiety and depression
- Ataxia; loss of physical coordination
- Memory loss and loss of cognition (dementia symptoms)
- Dystopia: muscle spasms
- Incontinence; bowel and urinary
What is the outcome of a prion disease and when does it usually occur?
Inevitably fatal and most die within a year of symptoms starting. NO cures, only treat the symptoms
Name four pathological characteristics of the brain due to a prion diseases
- Neuronal death (loss of neurones) leading to spongiform appearance of the brain (white gaps in the brain where the neurones were)
- Proliferation of astrocytes and microglia: acting like the immune cells of the brain to clear up the dead cells and compartmentalize the problem - but are only high in a diseased brain
- Build up of amyloid plaques (PrPscs) made of aggregated prions making protein lumps
- Evidence of oxidative stress
How common are prion diseases? List the three mechanisms in which they can occur from most-least common and when the onset of symptoms tends to occur for each
Very rare
- Sporadic (spontaneous): symptoms develop between ages 60-65
- Genetic: symptoms usually develop in early 50s and have longer duration
- Acquired (transmitted/infectious); iatrogenic, Kuru (canabolism) and vCJD (likely via consumption of beef products)
Name three examples of genetic prion diseases
- Creutzfeldt-Jakob disease (CJD)
- Fatal familiar Insomnia
- GSS
Different forms of the prion affects different parts of the brain and has slightly different characteristics. Specify where prions accumulate in the brain for the following prion diseases
A) CJD
B) FFI
C) Kuru
A) the cerebral cortex
B) thalamus
C) Cerebellum
List 3 differences and 4 similarities between CJD and Alzheimer’s
Similarities:
- Neurodegenerative diseases
- Similar clinical symptoms including dementia
- Linked high levels of oxidative stress
- Both have buildup of misfolded proteins in amyloid fibres or plaques
Differences:
- AD is much more common
- Involve different proteins (PrP vs amyloid-beta)
- Prions are transmissible
Describe what composes an amyloid plaque in prion diseases. Name five other neurodegenerative diseases where protein aggregates occur in the brain and name the appropriate protein or defect for each. Which is similar to CWD?
Aggregates of proteins which stack up to make fibrils/fibres and clump together to make an amyloid plaque. All proteins that aggregate are beta sheet rich
- Parkinson’s: a-synuclein
- Huntington’s: huntingtin
- Wilson’s: defects in copper metabolism (similar to CWD)
- Amyotrophic lateral sclerosis: defects in superoxide dismutase
- Alzheimer’s: amyloid beta proteins
What differs prion diseases from other neurodegenerative diseases and what causes this?
They’re transmissible: Injections of diseased brain tissue of one animal into the brain of another of the same species transmits the disease. However, this is not a normal pathway for infection, which suggests that the infectious agent in the TSEs is a protein
What age group was most affected by vCJD and what other prion disease was it related to?
Younger; median onset was 26, related to BSE/mad cow disease
Why is it unlikely that prion diseases are transmitted through viruses?
Treating the brain tissue with nucleases which destroy viral nucleic acids does not reduce their infectiousness
What does PRPres mean and what does it refer to?
Refers to the PRPsc because this protein is particularly resistant to conditions that would normally destroy proteins (i.e proteases, heat, strong alkaline conditions only have a limited affect)
What are the two major routes of transmission? (Including the four iatrogenic routes)
- Ingestion - through GI system (specifically the region of the gut with peyer’s patches/high immune function)
- Iatrogenic: corneal grafts, dura mater grafts, human derived growth hormone injection (hGH), experimental transmission in animal models
How does the immune system respond to prions and how do they reach the CNS?
They’re detected but don’t raise a large immune response. They evade the immune system’s response to break them down (resistant to proteolysis) and replicate in lymphoid tissue. A lot of lymphoid tissue is innervates by the ANS, and this provides a route for prions to enter the CNS.
Which type of lymphoid tissue seems particularly able to harbour the prion?
Follicular dendritic cells
Describe the process of how the prion protein replicates
*including
There’s a normal cellular form of the prion protein (PRPc), which every brain expresses highly at the synapses of neurones and in follicular dendritic cells - it’s coded by a gene on chromosome 20 and it has a largely unknown function. The PRPsc (prion protein) shares the same amino acid sequence as physiological PRPc, (it’s just a little shorter), and it can catalyze the conversion of PRPc to the prion. This results in exponential creation of PRPsc in the brain.
Name the changes of a PRPc once it has been converted to a PRPsc
It becomes extracellular, protease resistant, aggregates (as it has a high beta sheet content), doesn’t bind to copper and is NOT easily decontaminated
What are the two main proposed mechanisms of PRPsc catalyzed conversion? What are both the models based on and what would they both explain?
- Temple directed refolding model
- Nucleation dependent polymerization model
Both are based on that you have the same amino acid sequence but a conformational change (change in the 3D structure)
Both would explain the long incubation period found in prion diseases
What do the template refolding model and nucleation dependent polymerization models suggest?
Template refolding model: That there is a big energy barrier to overcome to convert PRPc to a prion, however once a small amount of prion is present it catalyzes the conversion with the formation of a heterodimer of the PRPc into more prion. From here, you only need a few prions to keep this going while the rest form amyloid plaques
Nucleation dependent polymerization model: suggests there is a low energy barrier and so a PRPsc can form more spontaneously, and slowly over time the pathogenic prion builds up to form amyloid fibres (individual monomers aren’t as important)
Name three things that describe how the formation of PRPsc leads to neurodegeneration
- PRPsc is cytotoxic
- A proposed function of PRPc is an antioxidant and when its converted into PRPsc that protection is lost
- Causes apoptosis and some necrosis of neurones (cleared by microglia) which leaves spongiform gaps
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