Scientists at the University of Cambridge have made a breakthrough in understanding how brain inflammation works in Alzheimer's disease. Their research reveals that large protein clumps trigger a unique, slow-moving immune response different from typical bacterial infections. The study focuses on how immune cells react to amyloid-beta aggregates, potentially explaining the chronic nature of neuroinflammation. These findings could pave the way for innovative treatments targeting the underlying mechanisms of dementia.
February 18, 2025
New insights into Alzheimer's brain inflammation: Study
"Small proteins could be acting like
bacteria in our brain and giving rise to neuroinflammation" - Arpan Dey,
University of Cambridge
Maryland, February 16: Brain inflammation,
while an important aspect of the immune response, plays a negative effect on
Alzheimer's disease. Unlike the acute, short-lived inflammation that fights
infection, the inflammation associated with Alzheimer's is chronic and
persistent. Scientists have been trying to figure out why this happens.
Key Points
1 New research explains unique inflammatory response
in Alzheimer's
2 Size of protein clumps critically affects immune
cell activation
3 Chronic brain inflammation differs from acute
bacterial responses
4 Study opens potential pathways for future dementia
treatments
New research reveals key differences in how
the brain's immune system responds to the disease compared to a bacterial
infection. The work is presented at the 69th Biophysical Society Annual Meeting
in Los Angeles.
The study focuses on how immune cells react
to amyloid-beta (Ab) plaques, a hallmark of Alzheimer's, and how this immune
response differs from the reaction to bacterial toxins. "Bacteria cannot
enter our brain because of the blood brain barrier," said Arpan Dey, PhD,
a postdoctoral associate in the lab of Professor David Klenerman at the
University of Cambridge in the United Kingdom. "But small proteins could
be acting like bacteria in our brain and giving rise to neuroinflammation,
which could be contributing to dementia," he added.
Dey and colleagues used a model system of
immune cells and exposed the cells to Ab aggregates or lipopolysaccharide (LPS),
a component of bacterial cell walls that triggers a strong immune response.
They focused on the formation of structures called myddosomes, which are
crucial for initiating inflammation.
The team discovered that larger Ab clumps
trigger more myddosome formation in immune cells. Smaller Ab clumps, even after
longer exposure, failed to trigger this response. This suggests that the size
of the Ab clump is critical for activating the immune system in Alzheimer's.
In contrast, LPS triggered a much faster and stronger
myddosome response than even the large Ab aggregates. This difference in timing
and intensity may explain why inflammation in Alzheimer's is chronic and
drawn-out, whereas the response to a bacterial infection is typically more
acute and resolves more quickly.
"Our findings reveal a crucial
distinction in how the brain's immune system reacts to a bacterial infection
versus Ab clumps," said Dey. "The slower, more sustained immune
activation by large Ab aggregates may contribute to the chronic inflammation
seen in Alzheimer's disease."
The team's next step is to start looking at
markers of myddosomes in blood samples from people with dementia and brain
samples from the UK Brain Bank.
By understanding the mechanisms driving
inflammation in Alzheimer's, they hope to contribute to the development of new
therapies that can specifically target the chronic inflammation associated with
the disease, potentially slowing its progression.
"This work opens up new avenues for drug
discovery," Dey said, he added, "by understanding and targeting the
pathways involved in the inflammatory response, we may be able to develop
treatments for Alzheimer's and other neurodegenerative diseases."
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