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$9.5 Million Federal Grant to Support Asthma Project with African-Americans
A Johns Hopkins-led team of experts in genetics, immunology, epidemiology and
allergic disease has embarked on a four-year effort to map the genetic code, or
whole genome, of 1,000 people of African descent, including men and women from
Baltimore.
Researchers say their initial goal is to find genetic variations underlying
asthma and to explain why the disease disproportionately afflicts blacks. As
much as 20 percent of African-Americans have asthma, a disease often associated
with allergies and marked by difficulty breathing, wheezing, coughing and
tightness in the chest. Chronic asthma can lead to serious lung damage, and
blacks are three times more likely to be hospitalized or die from the condition
than other American adults.
Study principal investigator and immunogeneticist Kathleen Barnes, Ph.D., says
the effort to sequence the genetic code of 500 asthmatics and 500 non-asthmatics
“represents an exciting opportunity to disentangle the genetic basis of a host
of other diseases, not just asthma, which have a hereditary component and
uniquely or disproportionately affect minorities.”
Barnes, a professor in the Division of Allergy and Clinical Immunology at the
Johns Hopkins University School of Medicine and the university’s Bloomberg
School of Public Health, and her team say they will make their findings freely
available to other researchers through the dbGAP national database of
genome-wide association studies, maintained by the National Library of Medicine,
a member of the National Institutes of Health (NIH). The National Heart, Lung
and Blood Institute, also part of the NIH, has provided the Johns Hopkins team
with $9.5 million in study funding.
For part of the initiative, the researchers have contracted with Illumina Inc.,
of San Diego, Calif., to create a commercially available, customized gene chip,
or DNA microarray test, dubbed the “African power chip,” to quickly find single
mutations in genetic materials from blacks that may be associated with
heightened disease risk.
Barnes says her team’s findings should fill in serious gaps in the hunt for
genetic variations posed by Illumina’s existing genotyping chip, and a similar
gene chip by Affymetrix Inc. of Santa Clara, Calif. Both chips were developed
from whole genome sequencing of predominantly white European men and women and
do not represent potential variations found mostly or only in minority groups.
“One of our biggest barriers as researchers trying to find the underlying
genetic roots of disease in minority groups has been the persistent lack of
microarray testing tools relevant to each racial profile, especially
African-Americans,” says Barnes, director of Johns Hopkins’ Genetics Research
Facility and its Lowe Family Genomics Core laboratory.
“Asthma is exacerbated by social factors, such as poverty, and inadequate
education and access to medical care,” adds Barnes, “so separating out the
genetic component is particularly complex, but scientifically doable.” Barnes is
also the Mary Beryl Patch Turnbull Scholar at Hopkins.
Researchers plan to sequence the genomes of blacks selected from among an
international group of people participating in existing genetic studies, who
have already been clinically diagnosed with asthma, or without, or who have
other kinds of compromised lung function, and whose family histories are well
documented. The participants will be selected from 15 academic research centers
across the United States, the Caribbean and South America, as well as from four
additional research sites in Western Africa.
An estimated 20 million Americans suffer from asthma, the most common chronic
condition among American children. Each year, more than 4,000 Americans die from
the condition, which also accounts for one-quarter of trips (some 2 million) to
hospital emergency rooms for breathing problems.
-Reprinted with permission of Johns Hopkins University School of Medicine
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