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High blood pressure in Older Adults linked
to gene
Newswise — Scientists have identified the
gene that sets off a sequence of events in
the blood vessels of otherwise healthy
adults that can lead to high blood pressure.
The disease process eventually makes
conditions in vessels ripe for the creation
of blockages that can cause heart attacks,
strokes and circulatory problems.
The finding in a study led by Ohio State
University researchers might lead to new
therapeutic options for high blood pressure,
especially hypertension associated with
aging. Obesity and aging contribute to
increasing cases of high blood pressure,
which currently affects an estimated 50
million Americans.
Despite more intensive treatments available
for hypertension, little has been done to
prevent it. A change in the structure of the
blood vessels, called vascular remodeling,
increases with age and triggers the onset of
the disease. When remodeling occurs, blood
vessel walls increase in thickness,
decreasing the diameter of the channel
through which blood normally flows.
The gene, called profilin 1, has been traced
to a series of interactions within the
smooth muscle cells of blood vessels that
causes those cells to increase in size. This
in turn narrows the channel through which
blood flows, causing stress on vessel walls,
injuring the lining of the vessel walls and
making it easier for blockages to develop.
By identifying this pathway, researchers
hope to pinpoint the most effective
therapeutic target to interfere with the
disease process.
The researchers used genetically altered
mice that produce excessive amounts of the
human profilin 1 gene in the vascular smooth
muscle cells and observed the changes to the
vessels that followed, which led to high
blood pressure by the time the mice were 6
months old – the rough equivalent to middle
age in humans.
“We created the disease in the animals and
then went backwards to understand how the
disease developed. This is an important
finding because vascular disease originates
in the smooth muscle cells, which have
significant impact on the dysregulation of
blood pressure that leads to heart disease,”
said Hamdy Hassanain, assistant professor of
anesthesiology at Ohio State University and
senior author of the study. Hassanain also
is an investigator in Ohio State’s Davis
Heart and Lung Research Institute.
The findings were published in the Dec. 28,
2007 issue of the Journal of Biological
Chemistry.
Blood vessels contain three important layers
– the endothelium that lines the vessel
walls, the smooth muscle cells responsible
for regulating blood flow, and the lumen,
the open channel through which blood
travels. In healthy young humans, the
production of compounds by the cells in
these layers remains balanced, allowing for
normal vessel function and unrestricted
blood flow.
Hassanain developed a transgenic mouse that
produces excess human profilin 1 in the
smooth muscle cell area with the intent to
cause stress in the vessel walls that leads
to hypertrophy, or an enlargement of the
smooth muscle cells that eventually leads to
structural and functional changes in the
entire vessel. The mice were developed to
test the theory that the impaired regulation
of the profilin 1 gene would eventually lead
to high blood pressure, and observe how that
happens.
“Vascular remodeling is a known problem as
people get older. Their blood vessels tend
to stiffen, even in healthy adults. This
causes stress on the vessels, which leads to
hypertension,” Hassanain said.
At the heart of the vessel activities is a
protein called actin within the smooth
muscle cells, and its relationship to
profilin 1. In the presence of too much
profilin1, actin is transformed from a
loosely configured protein into a more rigid
fibrous state. This change in actin’s nature
increases the size and the stiffness of
smooth muscle cells.
The cells undergo other changes that prepare
them for cell division, but under these
conditions, the vessel lining releases a
substance, nitric oxide, that won’t allow
the cells to divide. The smooth muscle
cells’ resulting growth pushes inward,
putting pressure on the lumen and
restricting blood flow, resulting in high
blood pressure.
“Profilin 1 is a tool that triggers events
that make the vessel more constricted and
leads to the signal that results in vascular
remodeling. Because we have understood the
pathway of the disease process, we might be
able to control vascular remodeling,”
Hassanain said.
Once a vessel is remodeled, more trouble is
typically ahead. Diseased vessels are often
characterized by injuries to the
endothelium, where the lining of the vessel
loses its protective layer. Once the lining
is injured and vulnerable, smooth muscle
cells will start to migrate inward, creating
sticking points for fats, debris and other
blood remnants.
“That’s the first hint of plaque. The smooth
muscle cell migration is the tip of the
iceberg of the plaque,” Hassanain said.
“We’re talking about all vessels, but when
we’re talking about this narrowing effect in
the brain, this could lead to stroke, and in
the coronary artery, it could lead to heart
attack. It’s all the same phenomenon.”
Other Ohio State co-authors of the study are
Mazin Alhaj, Maqsood Chotani, Zeinb
Aboelnaga, Mohamed Hassona, Gerard Nuovo and
Jay Zweier, all of the Davis Heart and Lung
Research Institute; Osama El-Sayed of
cardiology; and Sheik Wisel of surgery;
additional co-authors are Mariana Morris of
Wright State University and Pascal
Goldschmidt-Clermont of the University of
Miami. First author Moustafa
Moustafa-Bayoumi completed his Ph.D. in
Hassanain’s lab at Ohio State and is now at
California State Polytechnic University.
