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Breakthrough in understanding Parkinson's disease

Date:
November 13, 2014
Source:
Trinity College Dublin
Summary:
The Parkin protein functions to repair or destroy damaged nerve cells, depending on the degree to which they are damaged, scientists have learned. People living with Parkinson's disease often have a mutated form of the Parkin gene, which may explain why damaged, dysfunctional nerve cells accumulate.
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FULL STORY

Scientists at Trinity College Dublin have made an important breakthrough in our understanding of Parkin -- a protein that regulates the repair and replacement of nerve cells within the brain. This breakthrough generates a new perspective on how nerve cells die in Parkinson's disease. The Trinity research group, led by Smurfit Professor of Medical Genetics, Professor Seamus Martin, has just published its findings in the peer-reviewed Cell Press journal, Cell Reports.

Although mutation of Parkin has been known to lead to an early onset form of Parkinson's for many years, understanding what it actually did within cells has been difficult to solve. Now, Professor Martin and colleagues have discovered that in response to specific types of cell damage, Parkin can trigger the self-destruction of 'injured' nerve cells by switching on a controlled process of 'cellular suicide' called apoptosis.

Using cutting-edge research techniques, the Martin laboratory, funded by Science Foundation Ireland, found that damage to mitochondria (which function as 'cellular battery packs') activates the Parkin protein, which results in one of two different outcomes -- either self-destruction or a repair mode. Which outcome was chosen depended on the degree of damage suffered by the cellular battery packs.

Importantly, these new findings suggest that one of the problems in Parkinson's disease may be the failure to clear away sick nerve cells with faulty cellular battery packs, to make way for healthy replacements. Instead, sickly and dysfunctional nerve cells may accumulate, which effectively prevents the recruitment of fresh replacements.

Commenting on the findings, Professor Martin stated: "This discovery is surprising and turns on its head the way we thought that Parkin functions. Until now, we have thought of Parkin as a brake on cell death within nerve cells, helping to delay their death. However, our new data suggests the contrary: Parkin may in fact help to weed out injured and sick nerve cells, which probably facilitates their replacement. This suggests that Parkinson's disease could result from the accumulation of defective neurons due to the failure of this cellular weeding process."

Professor Martin also added: "We are very grateful for the support of Science Foundation Ireland, who funded this research. This work represents an excellent example of how basic research leads to fundamental breakthroughs in our understanding of how diseases arise. Without such knowledge, it would be very difficult to develop new therapies."


Story Source:

Materials provided by Trinity College Dublin. Note: Content may be edited for style and length.


Journal Reference:

  1. Richard G. Carroll, Emilie Hollville, Seamus J. Martin. Parkin Sensitizes toward Apoptosis Induced by Mitochondrial Depolarization through Promoting Degradation of Mcl-1. Cell Reports, 2014; DOI: 10.1016/j.celrep.2014.10.046

Cite This Page:

Trinity College Dublin. "Breakthrough in understanding Parkinson's disease." ScienceDaily. ScienceDaily, 13 November 2014. <www.sciencedaily.com/releases/2014/11/141113140042.htm>.
Trinity College Dublin. (2014, November 13). Breakthrough in understanding Parkinson's disease. ScienceDaily. Retrieved March 18, 2024 from www.sciencedaily.com/releases/2014/11/141113140042.htm
Trinity College Dublin. "Breakthrough in understanding Parkinson's disease." ScienceDaily. www.sciencedaily.com/releases/2014/11/141113140042.htm (accessed March 18, 2024).

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