The
gene1 mutation2 that causes Huntington's disease appears in every cell in the body, yet kills only two types of brain cells. Why? UCLA scientists used a unique approach to switch the gene off in individual brain regions and zero in on those that play a role in causing the disease in mice. Published in the April 28 online edition of Nature Medicine, the research sheds light on where Huntington's starts in the brain. It also suggests new targets and routes for
therapeutic3 drugs to slow the
devastating4 disease, which strikes an estimated 35,000 Americans.
"From day one of conception, the mutant gene that causes Huntington's appears everywhere in the body, including every cell in the brain," explained X. William Yang, professor of
psychiatry5 and biobehavioral sciences at the Semel Institute for Neuroscience and Human Behavior at UCLA. "Before we can develop effective strategies to treat the
disorder6, we need to first identify where it starts and how it
ravages7 the brain."
Huntington's disease is passed from parent to child through a mutation in a gene called huntingtin. Scientists blame a
genetic8 "stutter" -- a repetitive stretch of
DNA9 at one end of the altered gene -- for the cell death and brain
atrophy10 that progressively deprives patients of their ability to move, speak, eat and think clearly. No cure exists, and people with aggressive cases may die in as little as 10 years.
Huntington's disease targets cells in two brain regions for destruction: the cortex and the
striatum(纹状体). Far more neurons die in the striatum -- a
cerebral11 region named after its striped layers of gray and white matter. But it's unclear whether cortical neurons play a role in the disease, including striatal neurons'
malfunction12 and death.
Yang's team used a unique approach to uncover where the mutant gene
wreaks13 the most damage in the brain.
In 2008, Yang
collaborated14 with co-first author Michelle Gray, a former UCLA postdoctoral researcher now at the University of Alabama, to engineer a mouse model for Huntington's disease. The scientists inserted the entire human huntintin gene, including the stutter, into the mouse genome. As the animals'
brains atrophied15(脑萎缩), the mice developed motor and psychiatric-like problems similar to the human patients.
In the current study, Yang and Nan Wang, co-first author and UCLA postdoctoral researcher, took the model one step further. They integrated a "genetic scissors" that
snipped16 off the stutter and shut down the
defective17 gene -- first in the cortical neurons, then the striatal neurons and finally in both sets of cells. In each case, they measured how the mutant gene influenced disease development in the cells and
affected18 the animals' brain atrophy, motor and psychiatric-like symptoms.
"The genetic scissors gave us the power to study the role of any cell type in Huntington's," said Wang. "We were surprised to learn that cortical neurons play a key role in
initiating19 aspects of the disease in the brain."