Abstract

Cytomegalovirus (CMV) infections acquired by very-low-birthweight (VLBW) infants are incompletely characterized. To examine CMV transmission in VLBW infants, we evaluated maternal DNAlactia, infant DNAemia, and presence of clinical disease in a blinded study in VLBW infants in our newborn intensive care unit (NICU). To examine these issues, 200 VLBW infants were enrolled in a surveillance study, with weekly breast milk and infant whole blood samples collected, as available. Virologic (breast milk and infant whole blood real time PCR) and immunologic (IgG, IgM, and IgG avidity) correlates were evaluated. A chart review examined whether infants had symptoms compatible with CMV disease. DNAlactia was identified in 65/150 (43%) of lactating mothers. Nine CMV infections were identified in 9/75 CMV-exposed infants (12% of exposed infants). A higher median breast milk viral load (DNAlactia) correlated with an increased likelihood of DNAemia (p = 0.05). Despite potential symptoms compatible with CMV infection, clinicians had not considered the diagnosis of CMV in 6/9 cases (66%). All of these infants had chronic lung disease at discharge. There was no correlation between IgG antibody titer or IgG avidity index and the likelihood of transmission or CMV disease. In conclusion, in VLBW infants receiving milk from seropositive mothers, CMV infections are commonly acquired, and are frequently unrecognized. Future studies are needed to determine whether routine surveillance for CMV of either breast milk or infant plasma is beneficial in preventing or recognizing infection.

Highlights

  • Introduction published maps and institutional affilHuman cytomegalovirus (CMV) is one of the most commonly encountered viral pathogens in newborn infants [1]

  • A total of 184 infants were born to 150 mothers with evaluable breast milk samples (164 mothers consented, but breast milk was unavailable for 14 mothers)

  • DNAlactia was identified in 65/150 = 43% of lactating mothers for whom comparisons could have been made

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Summary

Introduction

Human cytomegalovirus (CMV) is one of the most commonly encountered viral pathogens in newborn infants [1]. Infection occurs in the context of transplacental transmission (congenital CMV), or post-natal transmission [2]. CMV infections, which are virtually always transmitted by breast-feeding, are ubiquitous and generally of little clinical significance in term babies. In premature infants, including very-low-birth-weight (VLBW;

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