What question did this study set out to answer?

This research aims to evaluate the inflammatory cytokine responses in children with critical bronchiolitis and explore the impact of viral types and clinical risk factors.

March 21, 2026

Viral and Host-Related Factors in the Nasal Inflammatory Response to Critical Bronchiolitis in Infants and Children

Key Result

Children with critical bronchiolitis exhibit a robust nasal inflammatory response with increased interferons and cytokines that is independent of the specific viral etiology.

Key Points

This research aims to evaluate the inflammatory cytokine responses in children with critical bronchiolitis and explore the impact of viral types and clinical risk factors.
Conducted a prospective cohort study in a PICU setting.
Analyzed nasal aspirates to measure cytokine levels using enzyme-linked immunosorbent assay.
Performed next-generation RNA sequencing on selected samples.
Compared inflammatory profiles among patients with different viral infections.
Patients displayed increased levels of type 1 and type 2 immunity-related cytokines.
No significant differences in cytokine levels between patients with rhinovirus and RSV infection.
Repeated bronchiolitis admissions were associated with lower inflammatory cytokine levels.
Next-generation sequencing revealed similar upregulation of pathways in rhinovirus and RSV patients compared to healthy controls, with downregulation of ciliary function genes.

Structured PICO

Population

Infants and children with critical bronchiolitis admitted to the PICU

Comparator

Healthy control patients

Outcome

Inflammatory cytokine response in nasal aspiratessurrogate

Critical bronchiolitis in children triggers a robust, virus-independent nasal inflammatory response characterized by upregulated proinflammatory pathways and downregulated ciliary function.

Main Result

Absolute Event Rate: 0% vs 0%

Abstract

Objectives: We aimed to evaluate the inflammatory cytokine response in children with critical bronchiolitis. Our secondary aims included: 1) understanding differences in inflammatory profiles between respiratory syncytial virus (RSV), rhinovirus, and polyviral infection, and 2) examining the association between clinical risk factors and the host inflammatory response. Design: A single-center, prospective cohort study of PICU patients with critical bronchiolitis. Setting: Medium-sized academic PICU from October 2021 to July 2024. Patients: Forty-two patients with critical bronchiolitis and nine healthy control patients. Interventions: None. Measurements and Main Results: Nasal aspirates were obtained and cytokines measured by enzyme-linked immunosorbent assay. The influence of viral type and host factors was assessed by nonparametric testing. In an exploratory analysis, cells from the nasal aspirates of a select group of patients underwent next-generation RNA sequencing (RNASeq). The nasal samples from patients with critical bronchiolitis exhibited an increase in interferons, type 1, and type 2 immunity-related cytokines. We did not identify differences in cytokine levels when comparing patients with rhinovirus to those with RSV infection. Patients with multiple (> 1) bronchiolitis admissions exhibited lower levels of inflammatory cytokines compared with patients during their first bronchiolitis admission. Using RNASeq, a subgroup of patients with rhinovirus or RSV exhibited similar upregulation of gene pathways associated with leukocyte chemotaxis, interferon signaling, and tumor necrosis factor superfamily cytokines compared with healthy controls. Pathways associated with ciliary function were downregulated compared with controls with RSV inducing a more pronounced downregulation than rhinovirus. Conclusions: These data demonstrate that patients with critical bronchiolitis exhibit a robust host inflammatory response independent of viral etiology. Our exploratory transcriptomic analysis showed upregulation of proinflammatory genes and downregulation of ciliary genes consistent with clinical characteristics of these patients at the bedside.

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