Study Discovers Novel Therapeutic Target for Acute Respiratory Distress Syndrome

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YouYang Zhao, PhD, the William G. Swartchild Jr. Distinguished Research Professor of Pediatrics in the Division of Critical Care, of Medicine in the Division of Pulmonary and Critical Care and of Pharmacology, was senior author of the study published in Science Translational Medicine.

A new Northwestern Medicine study has discovered a novel therapeutic target and therapeutic agents for older patients with acute respiratory distress syndrome (ARDS), according to recent findings published in Science Translational Medicine.

Approximately 190,000 Americans are diagnosed with ARDS every year, according to the American Lung Association. The disease occurs when fluid leaks into the lungs, depriving the lungs of oxygen entering the bloodstream. ARDS is commonly the result of injury to the lungs, but aging is also a major risk factor and increases the risk of mortality.

Despite advancements in the understanding of ARDS, there are no targeted therapies currently available for patients and the mortality rate remains high — approximately 40 percent.

“Compared to young adults, the incidence of ARDS resulting from sepsis, pneumonia, and COVID-19 in the elderly is as much as 20-fold greater and mortality is up to 10-fold greater,” said YouYang Zhao, PhD, the William G. Swartchild Jr. Distinguished Research Professor of Pediatrics in the Division of Critical Care and senior author of the study.

Using genetic lineage tracing in both aged and young mouse models of ARDS, Zhao’s team found that persistent lung injury and high mortality after sepsis due to ARDS were caused by impaired regeneration of endothelial cells in the lungs — cells that line blood vessels in the lungs to regulate the exchange of oxygen between the bloodstream and surrounding tissue — and lung repair.

Specifically, the expression of the gene FOXM1, a previously known mediator of endothelial cell regeneration, was impaired in the lungs of aged mice but not in younger mice.

“Employing an endothelium-targeted nanoparticle to deliver FOXM1 to the vascular endothelial cells in aged mice could reactivate the regenerative and reparative program and promote survival after sepsis,” said Zhao, who is also a professor of Medicine in the Division of Pulmonary and Critical Care and of Pharmacology.

To validate their findings, the investigators administered the FDA-approved chemotherapy drug decitabine in the aged mice, discovering that the drug reactivated endothelial cell regeneration, reversed impaired resolution of lung injury and increased overall survival.

The investigators also obtained samples of lungs infected with COVID-19 from elderly and middle-aged patients. They discovered that FOXM1 expression in lung endothelial cells from patients 80 years and older was not induced while in samples from patients aged 50 to 60 years, FOXM1 expression was markedly induced.

The findings point to FOXM1 as a promising therapeutic target for elderly patients with ARDS, according to Zhao.

“The delineation of the molecular mechanisms of aging-impaired endothelial regeneration is most important, which could lead to novel therapeutic strategy and agents for potential treatment of ARDS in elderly patients,” Zhao said.

This work was supported in part by National Institutes of Health grants R01HL123957, R01HL125350, R01HL133951, R01HL140409, R01HL148810, R01HL162299, R01HL164014 and R00HL145113.