November 24, 2014

Targeting Parkinson鈥檚 Disease Pathways

At a Glance

  • By blocking mitochondria division, scientists were able to restore function and protect neurons from damage in mouse models of Parkinson鈥檚 disease.
  • These preliminary research findings suggest a strategy to slow or halt the disease.
Mitochondia Mutant Drp1(left) blocks mitochondrial fission, resulting in longer mitochondria (arrow). Fis1 (right) promotes fission, resulting in smaller mitochondria.

Parkinson鈥檚 disease develops when brain cells that produce the neurotransmitter dopamine begin to die. Loss of these neurons, and others, leads to involuntary shaking, slowed movements, muscle stiffness, and other problems. Medications can help manage symptoms, but there's no treatment to slow or stop the disease.

The underlying causes of neuron death in Parkinson鈥檚 disease aren鈥檛 well understood. Recent studies have linked dysfunctional mitochondria as one of the pathways causing neuron death. These organelles convert compounds derived from food into the molecules that cells use for energy. Studies suggest that proteins involved in the dynamics of these organelles鈥攈ow they divide (fission), combine (fusion), and move鈥攎ay play a role in Parkinson鈥檚 disease.

A team led by Dr. Kim Tieu, who was at the University of Rochester School of Medicine and is now at Plymouth University in the UK, explored the effects of manipulating mitochondrial dynamics in 2 mouse models of the disease. One was a genetic model; another used a neurotoxicant that affects mitochondria. The work was funded by NIH鈥檚 最新麻豆视频 Institute of Environmental Health Sciences (NIEHS), 最新麻豆视频 Institute on Aging (NIA), and others. Results appeared in Nature Communications on November 5, 2014.

The scientists tested the effects of blocking or promoting mitochondrial fission by using genetic engineering techniques. To block fission, they used a mutant version of dynamin-related protein 1 (鈥婦rp1), a protein involved in fission. To promote fission, they boosted levels of Fission-1 (鈥婩is1), which helps bring Drp1 to mitochondria.

The Drp1 mutant restored dopamine release and protected neurons in both mouse models, while Fis1 did not. To confirm that blocking mitochondrial fission was causing these benefits, the researchers tested a small molecule called Mitochondrial Division Inhibitor-1 (Mdivi-1). Mdivi-1 is a Drp1 inhibitor that鈥檚 been shown to block mitochondrial fission. They found that Mdivi-1 also restored dopamine release and protected neurons in the mice.

By the time people are diagnosed with Parkinson鈥檚 disease, there鈥檚 already substantial neuron damage. Thus, the researchers tested the effects of delaying gene or drug delivery until after nerve damage had occurred. They found that 鈥媘utant Drp1 and 鈥媘divi-1 both improved dopamine release even after damage to the neuron pathway responsible for dopamine release. The findings suggest that the underlying cellular pathway that causes Parkinson鈥檚 disease might be restored even after neuron damage has progressed.

鈥淥ur findings show exciting potential for an effective treatment for Parkinson鈥檚 disease and pave the way for future in-depth studies in this field,鈥 Tieu says. 鈥淚t鈥檚 worth noting that other researchers are also targeting this mitochondrial fission/fusion pathway as potential treatments for other neurological diseases such as Alzheimer's disease, Huntington's disease, and amyotrophic lateral sclerosis.鈥

鈥攂y Harrison Wein, Ph.D.

Related Links

References:  Rappold PM, Cui M, Grima JC, Fan RZ, de Mesy-Bentley KL, Chen L, Zhuang X, Bowers WJ, Tieu K. Nat Commun. 2014 Nov 5;5:5244. doi: 10.1038/ncomms6244. PMID: 25370169.

Funding: NIH鈥檚 最新麻豆视频 Institute of Environmental Health Sciences (NIEHS), 最新麻豆视频 Institute on Aging (NIA), 最新麻豆视频 Center for Advancing Translational Sciences (NCATS), and 最新麻豆视频 Center for Research Resources (NCRR); and the Medical Research Council (UK).