Dong Qu, Vanessa Preuss, Lars Hagemeier, Lena Radomsky, Kerstin Beushausen, Jana Keil, Schaumann Nora, Benedikt Vennemann, Christine S Falk, Michael Klintschar
Pediatric research 2024 MarSudden infant death syndrome (SIDS) has been considered to be triggered by a combination of underlying immune dysregulation and infections. The thymus is a crucial lymphatic organ responsible for T cell development in infancy. We hypothesized that an altered thymic immune status may be detectable by intrathymic cytokine profiling in SIDS. 27 cytokines in protein lysates of thymus tissue and thymus weights were assessed in 26 SIDS cases and 16 infants who died of other reasons. Seventeen out of 27 cytokines were increased in thymic tissue of SIDS compared to controls without infections, and the most significant discrepancy was in infants younger than 20 weeks. The thymic cytokine profiles in SIDS cases were similar to those in controls with severe infection; however, the magnitude of the cytokine concentration elevation in SIDS was less pronounced, indicating sub-clinical infections in SIDS. In contrast to SIDS, intrathymic cytokine concentrations and thymus weight were increased with age in control children. Elevated thymic cytokine expression and thymus weight, as well as impaired age-related alterations in SIDS, may be influenced by subclinical infection, which may play a role in initiating SIDS in infants with a compromised immune response. Increased thymic weight and cytokine concentration may suggest possible subclinical infection in SIDS. Elevated thymic weight and cytokine concentration mainly in SIDS cases aged <20 weeks. Age-related impairment in the thymic weight and cytokine expression may be impaired by subclinical infection in SIDS. © 2023. The Author(s).
Dong Qu, Vanessa Preuss, Lars Hagemeier, Lena Radomsky, Kerstin Beushausen, Jana Keil, Schaumann Nora, Benedikt Vennemann, Christine S Falk, Michael Klintschar. Age-related cytokine imbalance in the thymus in sudden infant death syndrome (SIDS). Pediatric research. 2024 Mar;95(4):949-958
PMID: 37679518
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