Seasonal Asthma Attack Relief For Youth
Reported March 28, 2011
(Ivanhoe Newswire) -- A drug that targets the antibody
immunoglobulin E (IgE), a key player in asthma, nearly
eliminated seasonal increases in asthma attacks and
decreased asthma symptoms among young people living in
inner city environments, a clinical trial sponsored by
the National Institutes of Health has found.
This investigational use of the drug omalizumab, sold
under the brand name Xolair, was conducted in eight U.S.
cities by the Inner City Asthma Consortium (ICAC), a
nationwide clinical trials network supported by the
National Institute of Allergy and Infectious Diseases (NIAID),
part of NIH. Additional support for this research was
provided by the NIH National Center for Research
Resources and Novartis Pharmaceuticals Corporation.
"We know that treatment based on NIH asthma guidelines
is generally effective in managing the disease, but many
patients still experience asthma attacks requiring
visits to emergency rooms and hospitalizations," which
NIAID Director Anthony S. Fauci, M.D., was quoted as
saying.
"The results of this study are extremely promising
because they show that the addition of omalizumab to the
NIH guidelines-based therapy for asthma offers improved
asthma control and the potential to decrease the burden
of this chronic disease in children and adolescents."
In the United States, asthma affects approximately 18
million adults and 7 million children under the age of
18. Symptoms include wheezing, coughing, chest tightness
and shortness of breath, any of which can be provoked by
viral infections, allergens and air pollution. The
number of asthma attacks rises in the spring and fall
seasons when more allergens are in the air and the
occurrence of respiratory viruses increases.
The study enrolled 419 children and youths, ages 6 to 20
years old, diagnosed with moderate to severe allergic
asthma lasting more than one year. The children came
from Boston, Chicago, Cleveland, Dallas, Denver, New
York City, Tucson, Ariz. and Washington, D.C. Nearly all
were minorities, including African-Americans (60
percent) and Hispanics (37 percent).
The primary goal of the study was to determine if adding
omalizumab to NIH guidelines-based asthma therapy
reduced the number of days that participants experienced
any asthma-related symptoms. Another aim was to find out
if the addition of omalizumab could also reduce the
number of severe asthma attacks.
In addition to standard therapy, half of the
participants were assigned at random to receive
omalizumab, and the other half a placebo. Drug or
placebo was delivered via an injection under the skin
every two to four weeks over the 60-week period of
study.
As the trial proceeded, participants returned to the
clinic every three months for evaluation of their
symptoms. As needed, their non-trial medications were
adjusted according to the NIH asthma treatment
guidelines.
At the end of the study, the investigators found that,
overall, children and adolescents who received
omalizumab had a 25 percent reduction in days with
symptoms and a 30 percent reduction in asthma attacks
compared with those who received placebo. Those who
received omalizumab also had a 75 percent reduction in
hospitalizations. Importantly, the spring and fall
increases in asthma attacks that were seen in the
participants receiving placebo were almost eliminated in
those participants receiving omalizumab.
"The spike in asthma attacks in the fall, which is
associated with colds and other viral airway infections,
disappeared in the kids in the omalizumab group," which
William Busse, M.D., the principal investigator of ICAC
and professor of medicine at the University of
Wisconsin-Madison, was quoted as saying.
"Because the drug specifically targets IgE, which is the
antibody responsible for allergies, our observations
show the possible interplay between allergies,
respiratory viruses and IgE in provoking asthma
attacks."
Children and adolescents who responded the best to
omalizumab had positive skin tests for cockroach allergy
and high levels of cockroach allergen in their homes. In
previous work by NIAID-supported researchers, the
combination of cockroach allergy and exposure to
cockroaches was found to be an important cause of
asthma-related illness and hospitalization.
Omalizumab is a humanized monoclonal antibody, a pure
form of a single protein, custom-made for use in humans,
which binds to and blocks the activity of IgE, an
important molecule in allergy. When allergens bind to
IgE on the surface of certain immune cells, these cells
release substances that cause allergic reactions. In the
airways, these substances trigger the muscles to
contract, trapping air inside the lungs and causing
difficulty breathing.
"We continue searching for therapeutic strategies to
reduce the enormous burden of asthma. Following on the
findings reported here, ICAC studies now under way will
help us to determine if adding omalizumab only during
the period before fall seasonal asthma symptoms occur,
rather than throughout the year, results in the same
successful disease management," which Daniel Rotrosen,
M.D., director of NIAID's Division of Allergy,
Immunology and Transplantation, which oversees the ICAC
program, was quoted as saying.
SOURCE: New England Journal of Medicine, March 17, 2011 |
