Scientists at Northwestern University in the US identified a link between Huntington's disease and dysfunction of the subthalamic nucleus, a component of the basal ganglia, a group of brain structures critical for movement and impulse control.
Huntington's disease is characterised by the progressive loss of nerve cells in the brain and affects about one in 10,000 people. This fatal disorder is caused by a hereditary defect in a single gene.
The debilitating symptoms of Huntington's disease typically manifest in adulthood and involve loss of motor and cognitive function, depression and personality changes.
From the point of onset, symptoms develop and intensify over the following 10 to 25 years until death, typically due to complications associated with the disease.
Also Read
"While research into Huntington's disease has focused on other parts of the basal ganglia, the subthalamic nucleus has been largely overlooked," said Bevan.
Using mice genetically engineered to carry the Huntington's disease gene, scientists discovered the electrical activity of the subthalamic nucleus was lost.
Impaired subthalamic activity was caused by anomalous receptor signalling, leading to defective energy metabolism and accumulation of damaging oxidants.
The researchers also found abnormalities in the subthalamic nucleus occur earlier than in other brain regions, and that subthalamic nucleus nerve cells progressively degenerate as the mice age, mirroring the human pathology of Huntington's disease.
Currently, there is no cure for Huntington's disease; treatment can only alleviate some of the symptoms.
A better understanding of aberrant brain receptor signalling that leads to nerve cell dysfunction could reveal a target for therapy, researchers said.
The study was published in the journal eLife.
Disclaimer: No Business Standard Journalist was involved in creation of this content