For some time, there has been speculation that glucose metabolism was
associated with Alzheimer’s disease, with some researchers going so far
as to call Alzheimer’s diabetes type 3. Researchers with the National
Institutes of Health’s National Institute on Aging conducted the largest study
so far on proteins related to Alzheimer’s and identified proteins and
biological processes that regulate glucose metabolism that are
associated with Alzheimer’s. The study was published in the journal Nature Medicine.
The study was part of the Accelerating Medicines Partnership for
Alzheimer’s Disease (AMP-AD). The investigators assayed the levels and
analyzed the expression patterns of more than 3,000 proteins in brain
and cerebrospinal fluid samples collected at centers across the U.S.
“This is an example of how the collaborative, open science platform
of AMP-AD is creating a pipeline of discovery for new approaches to
diagnosis, treatment and prevention of Alzheimer’s disease,” said
Richard J. Hodes, NIA director. “This study exemplifies how research can
be accelerated when multiple research groups share their biological
samples and data resources.”
The study involved analyzing protein expression patterns in more than
2,000 human brain and almost 400 cerebrospinal fluid samples taken from
both healthy individuals and Alzheimer’s patients. They analyzed how
the protein modules relate to Alzheimer’s and other neurodegenerative
diseases. They observed changes in proteins related to glucose
metabolism and an anti-inflammatory response in glial cells in brain
tissues from both Alzheimer’s patients and people with documented brain
pathology who were cognitively normal. This also would seem to support
increasing evidence that brain inflammation is involved in the disease
as well.
In Alzheimer’s patients, they found that how cells extract energy
from glucose is increased in both the brains and spinal fluid of
Alzheimer’s patients. The proteins observed were also elevated in
preclinical Alzheimer’s patients, which is to say, people with brain
pathology of the disease who had not shown cognitive decline.
They also noted the importance of their findings that the glucose
metabolism/glial protein module was populated with proteins already
identified as genetic risk factors for Alzheimer’s.
“We’ve been studying the possible links between abnormalities in the
way the brain metabolizes glucose and Alzheimer’s-related changes for a
while now,” said Madhav Thambisetty, investigator and chief of the
Clinical and Translational Neuroscience Section in the NIA’s Laboratory
of Behavioral Neuroscience. “The latest analysis suggests that these
proteins may also have potential as fluid biomarkers to detect the
presence of early disease.”
Earlier research by Thambisetty and colleagues at Emory University
identified a connection between problems in how the brain breaks down
glucose and the amount of amyloid plaques and tangles were in the brain,
as well as memory and cognitive issues.
“This large, comparative proteomic study points to massive changes
across many biological processes in Alzheimer’s and offers new insights
into the role of brain energy metabolism and neuroinflammation in the
disease process,” said Suzana Petanceska, program director of NIA
overseeing the AMP-AD Target Discovery Program. “The data and analyses
from this study has already been made available to the research
community and can be used as a rich source of new targets for the
treatment and prevention of Alzheimer’s or serve as the foundation for
developing fluid biomarkers.”
The research group was led by Erik C.B. Johnson, Nicholas T. Seyfried
and Allan Levey at the Emory School of Medicine in Atlanta. The brain
samples were from autopsies of participants in various Alzheimer’s
research centers, including the Baltimore Longitudinal Study of Aging
(BLSA), Religious Orders Study (ROS) and Memory and Aging Project (MAP),
and Adult Changes in Thought (ACT) initiatives.
Samples from people with six other neurodegenerative disorders and
normal controls were provided by the Emory Goizueta Alzheimer’s Disease
Research Center, with data from the AD Knowledge Portal, the data
repository for the AMP-AD Target Discovery Program, and other NIA
projects.
https://www.biospace.com/article/glucose-metabolism-linked-to-alzheimer-s-disease/
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