Mitochondrial network (green fluorescence) in a blood vessel endothelial cell Credit: Jalees Rehman

In a new peer-reviewed publication, University of Illinois at Chicago researchers describe how the body's response to inflammation, which helps to fight many kinds of infections, also can counterproductively suppress much-needed cell repair and regeneration in blood vessels.

In the study, which is published in Immunity, the researchers describe an enzyme that blocks the ability of blood vessel cells to self-heal. By studying mice with sepsis—a condition caused when the body's inflammatory response to a bloodstream bacterial infection spirals out of control—they found that removal of the enzyme allows cells to fully regenerate.

"When cells are faced with an injury or an infection, it seems that they make a 'fight' or 'fix' choice," said UIC's Asrar Malik, senior author of the study and the Schweppe Family Distinguished Professor and head of pharmacology at the College of Medicine. "Inflammation is the 'fight' response, and the cells appear to delay while amplifying the ."

"We think that over time cells have evolved to favor fighting an infection over repairing damaged cells, but in some cases, this preference to fight puts the body at further risk," said Dr. Jalees Rehman, co-senior author and UIC professor of medicine, pharmacology and bioengineering at the College of Medicine. "Especially when the immune response of the body to an is so excessive that it damages such as the lungs, it is absolutely vital that we learn how to help cells restore their ability to regenerate and resolve the inflammation."

Rehman said that the enzyme—named cGAS—acts as a DNA sensor that is being activated by the DNA released by damaged mitochondria of the blood vessel .

"We showed that when the sensor is removed, blood vessel shift their balance towards restoration and regeneration," Rehman said.

In an experimental model of bacterial sepsis, mice lacking this DNA sensor had much higher rates of survival and showed rapid regeneration of the in the lung.

"It's possible that the degree to which this DNA injury sensor gets activated contributes to why some individuals survive a severe condition like sepsis," he said. "Suppression of regeneration is especially concerning in the elderly. Our study suggests that further study of this DNA sensor might provide provocative new areas for research to improve endogenous regeneration."

More information: Long Shuang Huang et al, mtDNA Activates cGAS Signaling and Suppresses the YAP-Mediated Endothelial Cell Proliferation Program to Promote Inflammatory Injury, Immunity (2020). DOI: 10.1016/j.immuni.2020.02.002

Journal information: Immunity