News — PITTSBURGH, April 13, 2021 – Wheezing, coughing that doesn’t stop, a pale and sweaty face: clinically, severe asthma attacks look very similar from patient to patient. But biologically, not all severe asthma is the same—and a team of scientists has, for the first time, identified the key difference in people, a finding that has important implications for treatment.
In a paper published today in , a group of scientists led by immunologists and pulmonologists at the , in collaboration with , used advanced tools of immunology, molecular biology and unbiased computational and bioinformatic approaches to characterize immune profiles of patients with severe asthma. These findings invite a new appreciation for the complexity of disease mechanisms and can lead to improved treatments.
“We started this study to better understand immune mediators of inflammation in asthma,” said lead author , clinical instructor of medicine at Pitt. “We found that despite being grouped broadly as ‘clinically severe,’ these asthma patients actually had very different and distinct immune profiles.”
is a debilitating condition that affects millions of people each year. According to the , 25 million Americans, or 1 in 13 people suffer from asthma. And while current standards of treatment—inhaled immunosuppressive corticosteroids, such as beclomethasone and budesonide—are effective in most patients, clinical markers that can help identify those who are likely to be resistant to treatment are lacking.
For patients who do not respond to standard corticosteroid treatment or respond to it poorly, there is no ‘one size fits all’ approach to treat severe disease. Because of that, while severe asthma accounts for 5 to 10 percent of all asthma cases, it consumes 50 percent of associated health care costs, amounting to $28 billion annually.
“Although breakthroughs in asthma therapy have greatly improved our ability to treat patients, many people still continue with disease that greatly diminishes their quality of life,” said co-senior author , director of , and chair of .
To characterize immune cells within the airways of severe asthma patients, the researchers, in collaboration with , director of the , used mass cytometry, RNA-sequencing and machine learning, and established a novel algorithm that links immune cells to cellular pathways potentially related to disease pathogenesis.
The research team found that lung aspirates from one group of patients were enriched with T cells polarized to fight infections, while the other group had a much lower level of T cells. At the same time, the second group had an increased number of innate immune cells expressing an inflammatory molecule IL-4—a cytokine known to be elevated in asthma.
“We have identified two clusters of severe asthma patients with very similar biomarkers but with strikingly distinct immune profiles and associated biological pathways,” said senior author , professor of medicine and immunology at Pitt. “These findings identify new targets for therapy, which are distinct in the two subgroups of severe asthma patients who otherwise would be indistinguishable based on biomarker profiles.”
“We believe that the cell types expressing IL-4 in the airways of one of the groups have not been previously identified in humans in any setting,” Ray added.
Researchers are optimistic that these findings will enhance precision medicine approaches to treating severe asthma patients.
“These important findings are the result of a successful team effort among physician-scientists and basic scientists across institutions that has established a new frontier in asthma research,” said Ray. “We hope the new knowledge gained will be used to develop new therapeutics to treat severe asthma patients and also allow improved stratification of patients for better efficacy of existing therapies.”
Other authors on the manuscript are Timothy Oriss, Ph.D., Qi Yan, Ph.D., Michael Gorry, Ph.D., William Horne, Ph.D., John Trudeau, Ph.D., Kathryn Scholl, Ph.D., Wei Chen, Ph.D., Prabir Ray, Ph.D., Florian J. Weisel, Ph.D., and Nadine Weisel, Ph.D., all of Pitt; Jay Kolls, Ph.D., of ; and Xiaoying Zhou, Ph.D., and Nima Aghaeepour, Ph.D., both of Stanford University.
This research was supported by the grants P01AI106684, R01HL113956, R01AI048927, U10HL109152, 1F32HL14741501, R01AI140134, R01HL118612, R01ES020926 and P01ES022849.
To read this release online or share it, visit .
# # #
About the University of Pittsburgh Schools of the Health Sciences
The University of Pittsburgh Schools of the Health Sciences include the schools of Medicine, Nursing, Dental Medicine, Pharmacy, Health and Rehabilitation Sciences and the Graduate School of Public Health. The schools serve as the academic partner to the UPMC (University of Pittsburgh Medical Center). Together, their combined mission is to train tomorrow’s health care specialists and biomedical scientists, engage in groundbreaking research that will advance understanding of the causes and treatments of disease and participate in the delivery of outstanding patient care. Since 1998, Pitt and its affiliated university faculty have ranked among the top 10 educational institutions in grant support from the National Institutes of Health. For additional information about the Schools of the Health Sciences, please visit .