('''TSEs''', also known as '''prion diseases''') are a group of progressive conditions that affect the
Brain and
Nervous System of
Human s and
Animal s and are transmitted by
Prion s. Mental and physical abilities deteriorate and myriad tiny holes appear in the
Cortex causing it to appear like a sponge (hence 'spongiform') when brain tissue obtained at
Autopsy is examined under a
Microscope . The disorders cause impairment of brain function, including memory changes, personality changes and problems with movement that worsen over time. Prion diseases of humans include classic
Creutzfeldt-Jakob Disease , new variant Creutzfeldt-Jakob disease (a human disorder related to
Mad Cow Disease ),
Gerstmann-Sträussler-Scheinker Syndrome ,
Fatal Insomnia and
Kuru . These conditions form a spectrum of diseases with overlapping signs and symptoms.
Unlike other kinds of infectious disease which are spread by
Microbe s, the infectious agent in TSEs is a specific
Protein called
Prion protein. Misshaped prion proteins carry the disease between individuals and cause deterioration of the
Brain . TSEs are unique diseases in that they can be inherited, occur spontaneously ("sporadic" TSE) or can be spread through infection (Collinge, 2001). Most TSEs are sporadic and occur in an animal with no prion protein mutation. Inherited TSE occurs in animals carrying a rare
Mutant prion
Allele , which expresses prion proteins that contort by themselves into the disease-causing
Conformation . Transmission occurs when healthy animals consume tainted tissues from others with the disease. In recent times a type of TSE called
Bovine Spongiform Encephalopathy (BSE) spread in
Cattle in an epidemic fashion. This occurred because cattle were fed the processed remains of other cattle, a practice now banned in many countries. The epidemic could have begun with just one cow with sporadic disease.
Prions cannot be transmitted through the air or through touching or most other forms of casual contact. However, they may be transmitted through contact with infected tissue, body fluids, or contaminated medical instruments. Normal
Sterilization procedures such as boiling or irradiating materials fail to render the pathogens non-infective.
Various zoo animals and pets have contracted TSEs, presumably through feed contaminated with tissues from infected cattle. In the laboratory, TSEs are transmissible to
Mice ,
Goat s and a wide range of other animals. (Collinge, 2001)
The degenerative tissue damage caused by human prion diseases (CJD, GSS, and kuru) is characterised by four features: spongiform change,
Neuron al loss,
Astrocytosis and
Amyloid plaque formation. These features are shared with prion diseases in animals, and the recognition of these similarities prompted the first attempts to transmit a human prion disease (kuru) to a
Primate in 1966, followed by CJD in 1968 and GSS in 1981.These neuropathological features have formed the basis of the
Histological diagnosis of human prion diseases for many years, although it was recognised that these changes are enormously variable both from case to case and within the
Central Nervous System in individual cases.
The clinical signs in humans vary, but commonly include personality changes, psychiatric problems such as
Depression , lack of coordination, and/or an unsteady gait (
Ataxia ). Patients also may experience involuntary jerking movements called
Myoclonus , unusual sensations,
Insomnia , confusion, or memory problems. In the later stages of the disease, patients have severe mental impairment (
Dementia ) and lose the ability to move or speak.
Early neuropathological reports on human prion diseases suffered from a confusion of nomenclature, in which the significance of the diagnostic feature of spongiform change was occasionally overlooked. The subsequent demonstration that human prion diseases were transmissible reinforced the importance of spongiform change as a diagnostic feature, reflected in the use of the term "spongiform encephalopathy" for this group of disorders.
Prions appear to be most infectious when in direct contact with affected tissues. For example, Creutzfeldt-Jakob disease has been transmitted to patients taking injections of
Growth Hormone harvested from human
Pituitary Gland s, and from instruments used for
Brain Surgery (Brown, 2000) (prions can survive the "
Autoclave " sterilization process used for most surgical instruments). It is also believed that dietary consumption of affected animals can cause prions to accumulate slowly, especially when
Cannibalism or similar practices allow the proteins to accumulate over more than one generation. An example is
Kuru , which reached epidemic proportions in the mid 20th century in the
Fore people of
Papua New Guinea , who used to consume their dead as a funerary ritual. Laws in developed countries now proscribe the use of
Rendered Ruminant proteins in ruminant feed as a precaution against the spread of prion infection in cattle and other ruminants.
Note that not all
Encephalopathies are caused by prions, as in the cases of
PML (caused by the
JC Virus ),
CADASIL (caused by abnormal NOTCH3 protein activity), and
Krabbe Disease (caused by a deficiency of the
Enzyme galactosylceramidase).
PSL -- which is a spongiform encephalopathy -- is also probably not caused by a prion, although the adulterant which causes it among
Heroin smokers has not yet been identified (
[http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=10563626&dopt=Abstract ,
[http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=11965173&dopt=Abstract ). This, combined with the highly variable nature of prion disease pathology, is why a prion disease cannot be diagnosed based solely on a patient's symptoms.
Mutations in the
PRNP Gene cause prion disease. Familial forms of prion disease are caused by inherited mutations in the PRNP gene. Only a small percentage of all cases of prion disease run in families, however. Most cases of prion disease are sporadic, which means they occur in people without any known risk factors or gene mutations. Rarely, prion diseases also can be transmitted by exposure to prion-contaminated tissues or other biological materials obtained from individuals with prion disease.
The PRNP gene provides the instructions to make a protein called the
Prion Protein (PrP). Normally, this protein may be involved in transporting copper into cells. It may also be involved in protecting brain cells and helping them communicate.
Mutation s in this gene cause cells to produce an abnormal form of the prion protein, known as PrPSc. This abnormal protein builds up in the brain and destroys nerve cells, resulting in the signs and symptoms of prion disease.
Familial forms of prion disease are inherited in an autosomal dominant pattern, which means one copy of the altered gene in each cell is sufficient to cause the disorder. In most cases, an affected person inherits the altered gene from one affected parent.
In some people, familial forms of prion disease are caused by a new mutation in the PRNP gene. Although such people most likely do not have an affected parent, they can pass the genetic change to their children.
These disorders are very rare. They affect about one person per million worldwide each year. Approximately 300 cases occur annually in the United States.
Recent research from the
University Of Toronto and
Caprion Pharmaceuticals have discovered one possible avenue which might lead to quicker diagnosis, a vaccine or possibly even treatment for prion diseases. The abnormally folded proteins which cause the disease have been found to expose a side chain of amino acids which the properly folded protein does not expose.
Antibodies specifically coded to this side chain amino acid sequence have been found to stimulate an immune response to the abnormal prions and leave the normal proteins intact.
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Another idea involves using custom
Peptide sequences. Since some research suggests prions aggregate by forming beta barrel structures, work done ''in vitro'' has shown that peptides made up of beta barrel-incompatible
Amino Acid s can help break up accumulations of prion.
- ''This entry incorporates public domain text originally from the National Institute of Neurological Disorders and Stroke, {Link without Title} ''
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