Potential Mechanism for Neurodegenerative Diseases Identified

Microbiology researchers at the University of Georgia studying a soil bacterium have identified a potential mechanism for neurodegenerative diseases.

A role for the protein HSD10 had been suspected in patients with Alzheimer’s disease and Parkinson’s disease, but no direct connection had previously been established. This new breakthrough suggests that HSD10 reduces oxidative stress, promotes cell repair and prevents cellular death.

The authors first discovered that an enzyme related to HSD10, CsgA, produces energy during sporulation in the bacterium Myxococcus xanthus. Spores enable cells to survive under nutrient-limiting conditions and can be thought of as the bacterial version of plant seeds. CsgA was found to degrade the phospholipid cardiolipin into fragments that were used as energy sources during sporulation much the same way humans produce and burn fat. Though normally a component of the lipid layer surrounding the cells, cardiolipin becomes dispensable as cells shrink to become spores.

The study was published Sept. 3 in the early online edition of Genes & Development.

In humans, this mechanism of cardiolipin degradation seems to have been appropriated for a different purpose. Cardiolipin is also found in mitochondria, where it surrounds and protects the energy-making machinery from oxidative stress.

HSD10 is a versatile protein with many known functions but its role in oxidative stress has remained a mystery. The authors showed that HSD10 preferentially degrades highly toxic cardiolipin peroxides, free radical produced during oxidative stress that would normally initiate apoptosis, or cell death.

HSD10 activity is strongly inhibited when bound to the amyloid beta peptide so prevalent in Alzheimer’s disease.

“Normally, apoptosis is beneficial for regulating multi-cellular systems,” said the study’s lead author Tye Boynton, a postdoctoral research associate in the Franklin College of Arts and Sciences. “But with rampant oxidative stress leading to uncontrolled cellular death, you end up with diseases such as Alzheimer’s and Parkinson’s. HSD10 potentially prevents this by removing these damaged lipids before they have a chance to act.”

Image of an alzheimer's brain.
A role for the protein HSD10 had been suspected in patients with Alzheimer’s disease and Parkinson’s disease, but no direct connection had previously been established. This new breakthrough suggests that HSD10 reduces oxidative stress, promotes cell repair and prevents cellular death. Image is for illustrative purposes only.

When cardiolipin becomes damaged by oxidative stress, the newly formed cardiolipin peroxides induce apoptosis instead of energy production. The UGA research team, led by microbiology professor Lawrence Shimkets, showed for the first time that HSD10 can mitigate oxidative damage.

“This research suggests that HSD10 prevents neurodegeneration by destroying cardiolipin peroxides and provides a fresh perspective on the etiology of Alzheimer’s disease that could inform novel drug strategies,” Shimkets said.

About this neurology and genetics research

Source: Alan Flurry – University of Georgia
Image Source: The image is in the public domain
Original Research: Abstract for “Myxococcus CsgA, Drosophila Sniffer and human HSD17B10 are cardiolipin phospholipases” by Tye O’Hara Boynton and Lawrence Joseph Shimkets in Genes and Development. Published online August 17 2015 doi:10.1101/gad.268482.115


Abstract

Myxococcus CsgA, Drosophila Sniffer and human HSD17B10 are cardiolipin phospholipases

Myxococcus xanthus development requires CsgA, a member of the short-chain alcohol dehydrogenase (SCAD) family of proteins. We show that CsgA and SocA, a protein that can replace CsgA function in vivo, oxidize the 2′-OH glycerol moiety on cardiolipin and phosphatidylglycerol to produce diacylglycerol (DAG), dihydroxyacetone, and orthophosphate. A lipid extract enriched in DAGs from wild-type cells initiates development and lipid body production in a csgA mutant to bypass the mutational block. This novel phospholipase C-like reaction is widespread. SCADs that prevent neurodegenerative disorders, such as Drosophila Sniffer and human HSD17B10, oxidize cardiolipin with similar kinetic parameters. HSD17B10 exhibits a strong preference for cardiolipin with oxidized fatty acids. This activity is inhibited in the presence of the amyloid β peptide. Three HSD17B10 variants associated with neurodegenerative disorders are inactive with cardiolipin. We suggest that HSD17B10 protects humans from reactive oxygen species by removing damaged cardiolipin before it induces apoptosis.

Myxococcus CsgA, Drosophila Sniffer and human HSD17B10 are cardiolipin phospholipases” by Tye O’Hara Boynton and Lawrence Joseph Shimkets in Genes and Development. Published online August 17 2015 doi:10.1101/gad.268482.115

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