PRINT
E-MAIL
THIS PAGE
CHAPTER
TEST 
LEARNING
OBJECTIVES HUNTINGTON'S DISEASE
Huntington's Disease (HD) is a fatal autosomal dominant condition that begins usually in the |
 |
| HD: Atrophy of the caudate and hydrocephalus ex vacuo | GFAP immunostain, showing gliosis. Left: HD; right: normal caudate nucleus |
The molecular abnormality of HD is CAG trinucleotide expansion of the huntingtin gene on chromosome 4p. This adds a polyglutamine segment to the huntingtin protein. This protein is widely expressed throughout the brain. It is thought that the CAG-expanded huntingtin has a toxic function. However, huntingtin is a key cellular protein involved in cellular transport and is important for cell viability. Therefore, loss of huntingtin function may also contribute to the pathogenesis of HD. The CAG triplet expansion is probably due to malfunction of cellular processes that repair strand breaks and remove mispaired bases from DNA. The expanded huntingtin, conjugated with ubiquitin, forms aggregates (inclusions) in the nuclei of affected neurons. These inclusions can be detected by immunohistochemistry using antibodies to huntingtin. These findings suggest that there is an error in the proteolytic degradation of the expanded huntingtin. Normally, this degradation takes place in cellular chambers called proteasomes and involves conjugation of huntingtin with ubiquitin. Impairment of this process apparently causes huntingtin-ubiquitin complexes to be translocated into the nuclei.
CAG repeats on other genes are also seen in spinobulbar muscular atrophy (Kennedy's disease), Machado-Joseph disease, an autosomal dominant ataxia seen mainly in Portugese of Azorean descent, and cerebellar degenerations. Paternally inherited HD shows the phenomenon of anticipation, i.e. the number of repeats increases in the offspring, resulting in earlier onset and more severe disease. Biochemical analysis of the striatum in HD shows loss of neurotransmitters, including GABA, acetylcholine and glutamate, which correlates with the loss of small neurons. Decrease of GABA and unbalanced dopamine activity result in chorea.
A rare form of chorea, beginning in adolescence or early adult life, is associated with an erythrocyte abnormality (chorea with acanthocytosis). Pathologically, this entity is similar to Huntington's disease but is caused by a different gene defect. Sydenham Chorea is a transient disorder in rheumatic fever caused by antibodies that react with neuronal antigens in the basal ganglia.
Further reading
Martinez-Vicente M, Sovak G, Cuervo AM. Protein degradation and aging. Exp Gerontol. 2005;40:622-33. PubMed
Updated: January, 2008
