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What's
New:
Imaging Damaged Brain Cells
in Living Mice Provides Alzheimer's Clues
New Orleans, Nov. 12, 2003 — Using recently developed
techniques for imaging individual cells in living animals,
a team led by researchers at Washington University School
of Medicine in St. Louis has watched as Alzheimer's-like
brain plaques damage mouse brain cells.
The results were presented at the 33rd Annual Meeting
of the Society for Neuroscience in New Orleans on Nov.
12.
"This work is very exciting," says principal
investigator David M. Holtzman, M.D. "We've been
able to visualize damaged nerve connections in living
animals and follow them over time in the same animal.
Our next step is to determine whether such damage is
reversible."
Holtzman is the Andrew B. and Gretchen P. Jones Professor
of Neurology and head of the Department of Neurology,
the Charlotte and Paul Hagemann Professor of Neurology
and a professor of molecular biology and pharmacology.
The first author is Robert P. Brendza, Ph.D., research
instructor in neurology.
The study was conducted in collaboration with Brian
Bacskai, Ph.D., investigator at Massachusetts General
Institute for Neurodegenerative Disorders and an assistant
professor of neurology at Harvard Medical School; and
Bradley Hyman, M.D., Ph.D., director of the Alzheimer's
Unit at the Massachusetts General Institute for Neurodegenerative
Disorders; and John B. Penney Jr. Professor of Neurology
at Harvard Medical School; William E. Klunk, M.D., Ph.D.,
director of psychiatry of the Alzheimer Disease Research
Center at the University of Pittsburgh; and Kelly Bales,
senior biologist, and Steven Paul, M.D., executive vice
president for science and technology at Eli Lilly and
Company.
In the 1990s, biologists discovered the protein that
makes certain jellyfish luminescent also could be used
to generate fluorescent cells in other species. By shining
light on a living mouse engineered to contain these
proteins, researchers can watch cellular activity over
time using a multiphoton microscope, a sophisticated
new microscope technique.
Holtzman's team used this technique to examine the brains
of mice that develop plaques similar to those characteristic
of Alzheimer's disease. The mice also were engineered
to have a subset of brain cells, or neurons, that express
yellow fluorescent protein. Using this model, they observed
neurons becoming increasingly disrupted by brain plaques
over time.
"We plan to use this system to further examine
the process of nerve cell damage and degeneration,"
Holtzman says. "This line of research should provide
new insight into the underlying processes involved in
the development of Alzheimer's disease and help us determine
whether the proteins that accumulate as brain plaques
are a useful and feasible target for Alzheimer's therapies."
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Brendza RP, Bacskai BJ, Simmons KA, Skoch JM, Klunk
WE, Mathis CA, Bales KR, Paul SM, Hyman BT, Holtzman
DH. Imaging dystrophy in vivo in fluorescent PDAPP transgenic
mice. Society for Neuroscience 33rd Annual Meeting.
Nov. 12, 2003.
Funding from the National Institutes of Health, the
Alzheimer's Association and Eli Lilly and Company supported
this research.
The full-time and volunteer faculty of Washington University
School of Medicine are the physicians and surgeons of
Barnes-Jewish and St. Louis Children's hospitals. The
School of Medicine is one of the leading medical research,
teaching and patient-care institutions in the nation.
Through its affiliations with Barnes-Jewish and St.
Louis Children's hospitals, the School of Medicine is
linked to BJC HealthCare.
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