News Release

Why is asthma worse in black patients?

Airway inflammation differs between races, study shows

Peer-Reviewed Publication

University of Illinois Chicago

African Americans may be less responsive to asthma treatment and more likely to die from the condition, in part, because they have a unique type of airway inflammation, according to a study led by researchers at the University of Illinois at Chicago College of Medicine.

Airway inflammation is a key component of asthma, and innovations in treatment are becoming more personalized based on the specific type of airway inflammation in a patient, says Dr. Sharmilee Nyenhuis, assistant professor of medicine at UIC and corresponding author on the study.

"Emerging evidence suggests that differences in airway inflammation can affect a patient's response to treatment, but whether the patterns of airway inflammation vary across race has, until now, been very unclear," said Nyenhuis, of UIC's division of pulmonary, critical care, sleep and allergy.

Black men and women are two to three times more likely than whites to be hospitalized or die from asthma. And while many factors contribute to the burden of asthma in African Americans--such as access to health care and environmental exposures--rates are disproportionate even when social and environmental elements are taken into account.

Nyenhuis and her colleagues performed a secondary analysis of more than 1,000 sputum samples obtained from AsthmaNet, a nationwide clinical research network created by the National Heart Lung and Blood Institute, and the Asthma Clinical Research Network. Samples of the coughed-up fluids were from past clinical trial participants over the age of 12 with mild or moderate persistent asthma and who had not smoked within the last year. The samples were tested for the presence of eosinophils--a type of white blood cell.

The study is one of the largest and most diverse trials conducted in the U.S. on race and asthma, with 26 percent of the patients self-identifying as African American. Researchers found that black patients were more likely to exhibit eosinophilic airway inflammation than whites, despite taking comparable doses of asthma medication, such as inhaled corticosteroids.

The results are published in the Journal of Allergy and Clinical Immunology.

"Our findings of higher numbers of African Americans with this type of airway inflammatory pattern suggests a mechanism that may account for more severe and difficult to control asthma in African Americans," said Nyenhuis. "It follows that the persistence of eosinophilic airway inflammation in African Americans may be associated with asthma exacerbations and an impaired response to corticosteroids."

The findings suggest that black patients with eosinophilic airway inflammation may not benefit from increasingly strong corticosteroid treatment--instead, other targeted therapies may need to be considered and researched as a treatment option for those black patients with difficult to control eosinophilic asthma.

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Co-authors on the paper from UIC include Dr. Jerry Krishnan, associate vice chancellor for population health sciences and professor of pulmonary, critical care, sleep and allergy; and Steven Ackerman, professor of biochemistry and molecular genetics.

Other authors on the paper are Dr. Alalia Berry of the University of Wisconsin; Dr. William Calhoun of the University of Texas; Vernon Chinchilli, Linda Engle, Erik Lehman and David Mauger of Pennsylvania State University; Dr. Nicole Grossman, Dr. Elliot Israel and Dr. Michael Wechsler of Brigham and Women's Hospital; Dr. Fernando Holguin and Dr. Sally Wenzel of the University of Pittsburgh; Rick Kittles and Dr. Monica Kraft of the University of Arizona; Dr. Stephen Lazarus of the University of California; Dr. James Moy of Stroger Hospital of Cook County; Dr. Stephen Peters of the Wake Forest School of Medicine; Dr. Wanda Phipatanakul of Boston Children's Hospital; Dr. Lewis Smith of Northwestern University; Dr. Kaharu Sumino of Washington University; Dr. Stanley Szefler of the Children's Hospital of Colorado; and Dr. Steven White of the University of Chicago.

This research was supported by the National Heart, Lung and Blood Institute, one of the National Institutes of Health (Grant Nos. U10 HL098096, U10 HL074225, U10 HLA074227, U10 HLA074231, U10 HLA074204, U10 HLA074212, U10 HLA074073, U10 HLA074206, U10 HLA074208, U10 HLA074218, R21 HL118588); the American Academy of Allergy, Asthma & Immunology/Association of Specialty Professors; the UIC Center for Clinical and Translational Science (Award No. KL2RR029878); and the National Center for Advancing Translational Sciences (Grant No. UL1TR000050).


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