Prions

Prions (from Proteinaceous Infectious Particles) are infectious particles made up only of a protein molecule. The prion theory was formulated in 1982 by Stanley Prusiner, who received the 1997 Nobel Prize. Prions are the cause of neurodegenerative diseases in humans and animals.

Characteristics of prions
In the human brain, under physiological conditions, the product of the PRNP gene on chromosome 20 is PrP (Prion Protein), specifically PrPC (C – cell) – a normal, wild-type form. Its physiological function is unclear, apparently involved in synaptic cell transmission and differentiation.

Pathogenic prions have the same primary structure (amino acid sequence), but differ in their conformational arrangement. While wild-type PrPC has a significant predominance of α-helix and only about 5% β-sheet, pathogenic PrPSc (Sc - scrapie [:scrapes:]) has a β-sheet content of up to 40%. Why aberrant PrPSc prions are formed is still the subject of a solution. There are several hypotheses for this.

Once an infectious prion is formed, it can "imprint" its conformation on neighboring, healthy prions. This probably spreads the disease to the tissues.
 * The VIRAL hypothesis assumes the participation of RNA viruses in the development of transmissible spongiform encephalopathies and thus in the development of infectious prions.
 * The MULTICOMPONENT hypothesis considers that binding with polyanions and lipids is necessary for the formation of infectious prions.
 * HEAVY METAL POISONING causes infectious prions when there is too little or less copper in the body, because a healthy amount of copper is needed for a healthy prion.

Pathogenic prions are extremely resistant to physical and chemical influences, which results in difficulties with sterilization (an experiment was made to burn the brains of affected animals at 600°C, about 1/3 of the exposed animals were infected with ashes). Highly infectious ones include the eye, brain and spinal cord tissue.

Diseases
Prion diseases are caused by pathogens, hat are the only ones that do not contain nucleic acid. They can be sporadic, genetic or infectious (even iatrogenic). The presence of defective proteins causes a condition collectively referred to as spongiform encephalopathy. It is a degenerative disease of the nervous system, in which the brain gradually acquires a spongy appearance due to the formation of miniature holes.

Human prion diseases

 * Creutzfeldt-Jakob Disease (CJD)
 * Sporadic CJD – has an incidence of 1-2 / 1,000,000. In the Czech Republic, more than 10 patients die from this form of CJD every year. Difficulties start around the age of 65. The disease progresses as a rapidly progressing dementia (in the range of 2-3 months), ataxia and myoclonus appear. The patient dies within 5-12 months of the first symptoms.
 * Iatrogenic CJD – occurred in patients treated with human growth hormone from cadaveric pituitary glands (now it is prepared recombinantly), by transmission of the dura mater, pericardium or cornea. There is also a risk of neurosurgical procedures transmitted by instruments. Prion transfer is probably also possible by transfusion.
 * Familial CJD – is a genetic form with a mutation in the PRNP gene and neuropsychiatric symptomatology.
 * A new variant of CJD – is characterized by psychiatric symptoms (anxiety, depression, behavioral changes), progressive cerebellar syndrome, myoclonus, chorea and other neurological symptoms. Unlike the sporadic form, the course is slower and affects younger age groups. Transmission is probably alimentary from meat of BSE animals. The incubation period is more than 10 years, about 200 people have died worldwide.
 * The contagion – occurred mainly in indigenous tribes in New Guinea who practiced ritual cannibalism. After several years of incubation, the patients developed tremor, ataxia, immobility, and subsequent death. After the suppression of cannibalism, the disease disappeared.


 * Alper's disease


 * Gerstmann-Sträussler-Scheinker syndrome


 * Fatal familial insomnia


 * Sporadic fatal insomnia

Animal prion diseases

 * Bovine spongiform encephalopathy (BSE) (mad cow disease)
 * Scrapie
 * Chronic wasting disease (CWD - chronic wasting disease)
 * Feline spongiform encephalopathy
 * Transmissive mink encephalopathy

Diagnostics
Diagnosis of spongiform encephalopathies is based on clinical and histopathological findings (immunohistochemistry, Western blot), or genetic examination.

The sporadic form of CJD is characterized by an EEG (looks like an EKG), on MR there is an obvious involvement of the basal ganglia and insula, atrophy of the frontotemporal area, and 14-3-3 protein in the cerebrospinal fluid. Familial CJD can be diagnosed by determining a mutation in the PRNP gene. Prior to the onset of a variant form of CJD prions can be detected in the tonsils, appendix, or spleen; MR involvement is mainly in the thalamus pulvinars, cerebrospinal fluid is negative for 14-3-3 protein.

Spongiform changes (optically empty spaces - appearance of a washing sponge), loss of neurons and proliferation of astrocytes (astrocytosis) can be found in the histological specimen.

Therapy
Causal therapy does not yet exist.

Relates articles

 * Causes of pathological conformation of proteins