AI Article Synopsis

  • Congenital CMV infection (cCMV) is the leading cause of congenital infections linked to long-term impairment, with unclear mechanisms behind this.
  • The study examined immune markers in blood samples from 99 children with cCMV and 54 without, finding that cCMV-infected neonates had fewer T cell receptor (TCR) excision circles but increased γδ T cells and B cells.
  • Children with more B cells at birth had better long-term health outcomes, indicating B cells may play a protective role in cCMV-related disease and highlighting their potential as a predictor for future health.

Article Abstract

Congenital CMV infection (cCMV) is the most common congenital infection that can cause long-term impairment (LTI). The pathogenesis of LTI is not completely understood. Fetal immunity may play a role in controlling the infection and preventing LTI, although immune activation may also contribute to fetal immunopathology. In this study, we analyzed various molecular markers of T and B cell numbers in neonatal dried blood spots of 99 children with cCMV and 54 children without cCMV: δRec-ψJα signal joints on TCR excision circles, intron recombination signal sequence k-deleting element signal joints on Igκ-deleting recombination excision circles, genomic intron recombination signal sequence k-deleting element coding joint, genomic Vδ1-Jδ1, and Vδ2-Jδ1 rearrangements. Of this cohort, clinical symptoms at birth and LTI at 6 y of age were recorded. Neonates with cCMV had fewer TCR excision circles in their blood than non-infected controls. Furthermore, cCMV infection was associated with increased numbers of γδ T cells and B cells, and these numbers were positively correlated with CMV viral load in the dried blood spots. Infected children with a better long-term outcome had higher numbers of B cells at birth than those who developed LTI; no difference in B cell replication was observed. The potential protective role of B cells in controlling cCMV-related disease and the clinical value of this marker as a predictor of long-term outcome merit further evaluation.

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http://dx.doi.org/10.4049/jimmunol.1601182DOI Listing

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