Washington University. US: Highlighting a potential target in the treatment of multiple sclerosis
(MS) and Alzheimer’s disease, new research suggests that triggering a
protein found on the surface of brain cells may help slow the
progression of these and other neurological diseases.
Working with mice, two research teams at Washington University School of Medicine
in St. Louis independently linked the protein to the ability to clear
debris from the brain. Such waste builds up both as a byproduct of daily
mental activities and as a result of misdirected immune system attacks
on brain cells. If too much debris is present in the brain for too long,
it can contribute to neurological disease.
In one study, appearing online Feb. 26 in Cell, scientists showed
that Alzheimer’s brain plaques build up more slowly in mice that have a
defective version of the TREM2 protein. In another, published Jan. 29
in Acta Neuropathologica, researchers showed that mice lacking the same
protein had trouble cleaning up debris in the brain produced by damage
to a protective coating on nerve cells. The problem is thought to occur
in MS and other neurological disorders.
“We’ve been very interested in identifying ways to control
naturally occurring mechanisms that help clean and repair the brain, and
these new studies provide clear evidence that TREM2 could be just such a
target,” said Laura Piccio, MD, PhD assistant professor of neurology
and senior author of one of the studies.
Scientists are looking for ways to activate the protein to slow or prevent damage caused by neurological disorders.
Previous studies have linked rare forms of the TREM2 gene to
early-onset dementia and increased risk of Alzheimer’s disease,
Parkinson’s disease and amyotrophic lateral sclerosis (ALS).
Scientists knew the protein was found on brain cells called
microglia, which help maintain and repair the central nervous system.
The new studies are among the first to provide clear evidence that the
protein plays an integral role in at least some of these processes.
In Alzheimer’s disease, amyloid beta, a byproduct of brain metabolism
that is normally cleared from the brain, builds up to form plaques.
Researchers in the laboratories of Marco Colonna, MD, the Robert Rock
Belliveau MD Professor of Pathology, and John Cirrito, PhD, associate
professor of neurology, bred mice lacking the gene with mice genetically
engineered to have an Alzheimer’s-like condition.
First author Yaming Wang, PhD, a postdoctoral research scholar,
monitored the buildup of amyloid plaques in the mice offspring as they
aged and found that the absence of the gene significantly accelerated
the accumulation of the plaques.
“We found that microglia cluster around amyloid plaques when TREM2 is
present, presumably because the cells are getting ready to absorb the
plaques and break them down,” said Colonna. “When TREM2 is absent, this
clustering does not occur.”
In MS, misdirected immune cell attacks damage myelin, a protective
coating on nerve cells, leaving myelin fragments in brain tissue.
Failure to promptly remove this debris can worsen damage caused by the
condition and inhibit repair mechanisms.
For the MS study, Piccio and colleagues at the John L. Trotter MS
Center at Washington University School of Medicine and Barnes-Jewish
Hospital gave a compound called cuprizone to mice that lacked the TREM2 gene. Cuprizone causes loss of myelin in a manner somewhat similar to that seen in people with MS.
“When we give normal mice this chemical, they can clear most of the
myelin fragments from the brain,” Piccio said. “But when we gave
cuprizone to mice that did not have the gene and looked at their brains
four, six and 12 weeks later, we could still see evidence of damaged
myelin.”
Motor coordination in these mice also was significantly more impaired
after cuprizone exposure. This may reflect enhanced damage to brain
cells resulting from the lingering presence of damaged myelin in the
brain.
Colonna and his colleagues showed that TREM2 detects molecules
associated with amyloid beta and with damaged neurons. They believe that
the protein helps keep microglia from self-destructing as debris is
cleared from the brain.
“This is a mechanism that is very common in immune cells,” he
explained. “When a signal activates immune cells and they start
attacking an invader or working to repair an injury, they start using
energy very rapidly. If the cells do not receive a second signal
confirming the need for their services, this increased energy usage will
kill them.”
Wang Y, Cella M, Mallinson K,
Ulrich JD, Young KL, Robinette ML, Gilfillan S, Krishnan GM, Sudhakar S,
Zinselmeyer BH, Holtzman DM, Cirrito JR, Colonna M. TREM2 lipid sensing
sustain microglial response in an Alzheimer’s disease model. Cell, online Feb. 26, 2015, http://dx.doi.org/10.1016/j.cell.2015.01.049
The research was supported by the Lilly Innovation
Fellowship Award; the Washington University Digestive Diseases Research
Core Center, grant P30 DK52574; the National Multiple Sclerosis Society;
the Knight Alzheimer’s Disease Research Center, pilot grant P50
AG005681-30; and the Cure Alzheimer’s Fund.
Cantoni C, Bollman B, Licastro D, Xie M, Mikesell R, Schmidt R, Yuede
CM, Galimberti D, Olivecrona G, Klein RS, Cross AH, Otero K, Piccio L.
TREM2 regulates microglial cell activation in response to demyelination
in vivo. Acta Neuropathologica, Jan. 29, 2015.
DOI 10.1007/s00401-015-1388-1
The research was supported by the Fondazione Italiana Sclerosi Multipla,
the National Multiple Sclerosis Society and the Dana Foundation.