Alzheimer’s disease present does not have a known cure or effective therapy. A recent study attempts to fill the gaps in our understanding of how the progressive neurodegenerative disorder arises in the brain.
According to a study by Flinders University, a protein called tau, a critical factor in the development of Alzheimer’s disease, turns from normal to a disease state.
The research also demonstrates how this discovery could deliver a therapeutic target.
Publish in the journal Science Advances, the team’s findings provide hope for preventing the tau transformation process from happening, thereby keeping tau in a healthy state and avoiding toxic effects on brain cells.
Senior study author Dr. Arne Ittner, Senior Research Fellow in Neuroscience in the Flinders Health and Medical Research Institute Said :
In the course of Alzheimer’s disease development, tau accumulates in deposits inside brain cells.
During this process, tau gets heavily modified, with various deposits made up of tau carrying multiple small changes at many different positions within the tau molecule.
While such changes to tau have known to neuropathologists for decades, it remain unclear how tau arrives at this multi-modified stage.
The new study has solve part of this mystery and provides a new mechanism to explain how tau gets progressively modified.
The study set out to answer whether one change at one specific spot in tau would make it easier for another spot to be modified.
The team focus on the relationship between tau and protein kinases, which are enzymes that introduce changes in tau.
Study lead author Dr Kristie Stefanoska, Research Fellow in Dementia at Flinders University Said :
The researchers conduct a large experiment that include up to 20 different changes in tau and 12 enzymes, focussing on the most abundant type of change seen in tau from the brains of Alzheimer’s patients.
And the study did discover that one change in tau does makes it easier for another change to be introduced, it was also able to identify “master sites” in tau, being specific spots that govern subsequent modifications at most of the other sites.
Dr. Arne Ittner Said :
The next step for the team was to see whether master sites could be target to reduce the toxic properties of tau in Alzheimer’s, in a bid to improve memory function.
The current study employe mice that have both amyloid and tau and develop Alzheimer’s-like symptoms, including memory deficits.
The researchers found that mice did not develop memory deficits when they had a version of tau that lack one of the identified master sites, compare with mice that had the usual version of tau.
The team will now investigate how its findings can be translate into a treatment.
Dr Kristie Stefanoska Said :
The authors say the new mechanism and the master sites at its centre could apply to a range of neurological disorders in which tau is involve, including Parkinson’s disease, concussion-induce chronic brain injury and stroke.
Dr. Arne Ittner Said :