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E-mail:
Dr.
Thomas Van Groen
CV:
Dr.
Thomas Van Groen CV
PubMed
Dr.
Thomas Van Groen publications on
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Behavioral Assessment Core
Dr. Thomas Van Groen
Associate Professor
UAB Cell Biology
Overview of Current Research
Amyloid
angiopathy in cognitive
dysfunction
and Alzheimer’s
disease
In
addition to the well-known
accumulation of amyloid beta (Aβ)
in neuropil plaques and
intracellular sites, Alzheimer’s
disease (AD) is associated with
substantial Aβ deposition
in the cerebral vasculature.
Whereas, clearly,
cerebrovascular disease is not
the sole cause of AD, mounting
evidence indicates that
cerebrovascular amyloid
angiopathy (CAA) contributes to
some aspects of the cognitive
impairments associated with AD.
These findings have led to the
hypothesis that CAA contributes
to neuronal dysfunction and thus
cognitive impairment, possibly
through brain hypoperfusion.
However, there is a temporal
overlap between the deposition
of Aβ in neuropil and
cerebrovasculature, making it
difficult to separate the
relative contributions to AD
dementia from CAA vs. neuropil Aβ.
Our recent preliminary studies
examining the course of
amyloidosis in AD model mice
indicate that CAA often develops
prior to neuropil Aβ
deposition. Further, some of the
available transgenic (Tg) AD
models exhibit quite different
levels of vascular versus
neuropil deposits. Finally,
neuropil Aβ develops more
extensively and earlier in
female vs male mice. Thus, the
following studies are designed
to use the temporal separation
and quantitative differences in
Aβ deposition in the blood
vessel wall versus neuropil, to
test the hypothesis that CAA
contributes to cognitive
dysfunction and pathology in
AD.
We are testing the prediction
that 1) CAA precedes neuropil Aβ
deposition and 2) compared to
the course of Aβ deposition
in neuropil, CAA is more closely
linked in time to the onset of
cognitive impairment. 3) We also
are examining the hypothesis
that Aβ deposition in blood
vessels is associated with
altered blood flow, oxidative
stress and inflammation that in
turn will lead to cognitive
deficits and finally, 4) we will
study whether pharmaceutical
reduction of cerebrovascular
inflammation significantly
reduces the development of CAA
and brain Aβ deposition and
attenuates the development of
cognitive dysfunction. We
propose to use simultaneous
quantification of CAA, and
extra- and intra-cellular Aβ
deposition, and cortical blood
flow in conjunction with
systematic analyses of
behavioral and pathological
markers in two different Tg AD
models (expressing high and low
degrees of CAA), to test these
working hypothesis.
The proposed studies will
produce the first systematic
time course study relating the
deposition of Aβ in the
vascular and other compartments
of the brain to development of
cognitive dysfunction. The
multidisciplinary experience of
our group in studies of
hippocampal system
anatomy/physiology, vascular
function and detailed behavioral
and pathological analyses in Tg
animals places us in an
advantageous position to test
the increasingly important
possibility that CAA is a
significant contributor to
cognitive dysfunction and
neuropathology in Tg AD models
and in humans.
Hypertension
in cognitive dysfunction and
Alzheimer’s disease
Hypertension is a risk factor
for stroke, cardiovascular
disorders, and vascular
dementia, and the incidence of
these diseases grows with
increasing blood pressure.
Recent studies have shown that
hypertension is also a risk
factor for Alzheimer’s disease
(AD). AD is associated with the
accumulation of amyloid beta (Aβ)
in plaques in the brain
parenchyma but also with
substantial amyloid β
deposition in the cerebral
vasculature. Furthermore, it has
been demonstrated that AD
patients have cerebral
hypoperfusion and hypoactivity.
Clearly, cerebrovascular disease
is not the sole cause of AD, but
mounting evidence indicates that
changes in the
cerebrovasculature and in
cerebral blood flow do
contribute to the cognitive
dysfunction associated with AD.
For instance, recent studies
have indicated that cerebral
blood vessel reactivity is
impaired in Tg AD model mice.
The brain renin-angiotensin
system plays an important role
in the regulation of the
cerebral blood pressure and
blood flow, but with increasing
age (and during the development
of CAA) this regulation is
altered. This modifies the
cerebral circulation such that
sustained hypoperfusion or
oligemia is impacted upon the
aging process to induce
augmented pathology. Our
preliminary studies indicate
that aged Tg AD model mice
exhibit decreased cerebral blood
flow and blood volume when
significant amyloid β
depositions are present.
Together, these findings have
led to the hypothesis that
sustained hypertension will lead
to decreased functional
hyperemia in the brain, and that
this contributes to brain
hypoperfusion which adds to the
cognitive impairments of AD.
Further, decreased blood flow
will concurrently lead to
increased amyloid β
deposition in the brain due to
decreased clearance of amyloid
β. Thus, our studies are
designed to test the hypothesis
that long-term untreated
hypertension will lead to
perturbed vascular function,
oligemia, and increased
cognitive dysfunction and
pathology in AD model
mice.
Thank
you for using the UAB
Neuroscience Behavioral
Assessment Core. Please give
appropriate acknowledgement to
P30 NS47466 in your papers.
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