MONDAY, June 30 (HealthDay News) -- A newly discovered molecular
malfunction may explain the development of high blood pressure,
diabetes and immune problems, researchers report.
Rogue versions of enzymes known as proteases roam the body,
clipping off working segments of the receptors that allow insulin
to enter cells and do its job, according to a report in the June 30
online issue of
Hypertension.
That uncontrolled enzymatic activity also reduces the immune
system's response to infection and raises blood pressure, the
report noted.
"We are describing a new mechanism for disease and injury to the
body," said study author Frank DeLano, a research scientist with
the department of bioengineering at the University of California,
San Diego. "It is an idea that hasn't been presented before. If we
apply a protease inhibitor, we can prevent the damage we see in
laboratory animals."
DeLano and his collaborator, Geert Schmid-Schonbein, a professor
of bioengineering at UCSD, have been working with a widely used
laboratory model of disease, a rat bred to have high blood
pressure.
They have found that proteases, whose function is to clear away
molecular debris, can go awry and split apart a number of different
cell wall receptors. If insulin receptors are damaged, normal
metabolism of glucose is not possible, and diabetes can be the
result. Proteases can also damage receptors that are vital for the
functioning of infection-fighting leukocytes.
The researchers also found that protein receptors on the surface
of cells are clipped off as the rats develop high blood pressure.
"Many receptors in blood vessels cause them to relax," DeLano said.
"Many proteases we see in the animals cleave receptors responsible
for relaxation." Giving the rats doxycycline, an antibiotic that is
also a protease inhibitor, brought down their blood pressure and
restored normal immune system function.
The proteases that cause the damage leak out of the intestine,
DeLano said. "The mechanism is a leaky or permeable intestine," he
said. "We call it leaky gut syndrome."
A major next step will be to show that the protease damage seen
in laboratory rats occurs in humans. "We will have to do human
trials," DeLano said. "We are working with other researchers on
human trials."
"This is really an important observation," said H. Glenn Bohlen,
a professor of cellular and integrative physiology at Indiana
University Medical School, who wrote an accompanying editorial. "It
ties in information that high blood pressure and insulin resistance
have the same cause, damage to receptors."
The function of proteases in rats and humans is the same, so
what has been seen in the laboratory rats likely occurs in people.
"It probably happens in humans on a different scale," Bohlen said.
"Rats live at a different metabolic rate, much faster than in
people."
The newly reported studies might also help explain why
antioxidants such as vitamins C and E help against inflammation, he
said.
"The next approach probably would be to treat an inflammatory
state," Bohlen said. "There is something going on that we can
interact with. There are many commercially available methods for
blocking proteases."
In addition to antibiotics such as doxycycline, drugs such as
ACE inhibitors are protease inhibitors, DeLano said. Protease
inhibitors are also used to control HIV, the virus that causes
AIDS.
More information
Importance of controlling blood pressure and diabetes is
described by the
American Heart Association.
