Researchers say they found that infection with a common virus that can be transmitted from mother to fetus before birth significantly worsens an often-fatal complication of premature birth called necrotizing enterocolitis (NEC) in experiments with mice.

Up to nearly 10% of premature infants develop NEC, a disease characterized by severe inflammation of the intestinal lining that ultimately kills this tissue. About a third of babies with NEC ultimately die from it, and survival rates have remained unchanged over the past three decades.

New Study:

The research team, led by Johns Hopkins Children’s Center investigators and funded by the National Institutes of Health, says the new findings advance the search for better treatments for NEC — a relatively rare condition, but still the most common emergency intestinal complication in preemies.

A report on the study was published on 13^th Feb in Cellular and Molecular Gastroenterology and Hepatology.

Recent research in animals, Hackam says, has shown that NEC’s trademark inflammation is at least partly due to a persistent uptick in an immune protein called toll-like receptor 4 (TLR4), which becomes activated by the abnormal accumulation of specific intestinal bacteria that tend to overgrow in the digestive tract of premature infants. But why NEC is more severe in some babies and tends to be spreadable has been a mystery.

That led to Cytomegalovirus (CMV) as a suspect, Hackam says.

Cytomegalovirus (CMV):

An estimated 40% to 80% of people worldwide are chronically infected with cytomegalovirus, a virus in the herpes family that doesn’t usually cause symptoms in healthy people but is a common cause of hearing loss and other organ-damaging birth defects when transmitted from mother to fetus during pregnancy. Fetuses acquire CMV from infected mothers during gestation in 30%–50% of cases.

Suspecting a connection between CMV and NEC severity, Hackam and his colleagues developed a neonatal mouse model of NEC with CMV. When they compared the intestines of the rodents with and without CMV infection, they found that mice harboring CMV had significantly worse tissue damage and higher mortality rates compared to those without this virus.

Molecular mechanism of CMV in animal model:

The researchers compared gene activity in the intestines of the two groups of mice. They found that CMV infection triggered genetic pathways that encouraged inflammation, disrupted metabolism and prompted cells to make more TLR4.

A closer look showed that CMV also damaged mitochondria, organelles that serve as cells’ energy factories. The damage significantly decreased mitochondrial production of adenosine triphosphate (ATP), a molecule that cells use for fuel.

Further experiments with mouse tissue, Hackam noted, showed that TLR4 was necessary for each of these effects. Mice genetically altered to produce no TLR4 in their intestines, for example, had significantly lower NEC severity even with CMV infection, suggesting that this protein could be a good target for developing drugs against NEC.

If animal and human studies confirm the CMV-NEC connection, another treatment option might be to administer adenosine, Hackam explains, a precursor for ATP that’s commonly sold as a dietary supplement. When the researchers gave mice with NEC and CMV adenosine, it significantly reduced NEC severity. The team plans to investigate these ideas in future studies.

Reference:

1. Scheese, Daniel, Peng Lu, Hannah Moore, Koichi Tsuboi, Cody Tragesser, Johannes Duess, Zachariah Raouf, et al. 2025. “Cytomegalovirus Worsens Necrotizing Enterocolitis Severity in Mice via Increased Toll Like Receptor 4 Signaling.” Cellular and Molecular Gastroenterology and Hepatology, no. 101473: 101473. https://doi.org/10.1016/j.jcmgh.2025.101473.

(Newswise/SD)