Phenotypic subgroups and classification criteria performance in pediatric Behcet’s disease: insights on systemic involvement
Paediatrics
Phenotypic subgroups and classification criteria performance in pediatric Behcet’s disease: insights on systemic involvement
Paediatrics

Phenotypic subgroups and classification criteria performance in pediatric Behcet’s disease: insights on systemic involvement

Rheumatology (Oxford). 2025 Nov 29:keaf637. doi: 10.1093/rheumatology/keaf637. Online ahead of print.

ABSTRACT

OBJECTIVES: Behçet’s disease (BD) is a multisystem vasculitis with variable pediatric presentations. Early diagnosis may be difficult due to heterogeneous manifestations and limited applicability of existing criteria. This study compared clinical characteristics by age at onset and examined factors contributing to diagnostic delay.

METHODS: A retrospective cohort of 38 pediatric BD patients from a tertiary center was analyzed. Patients were grouped as early-onset (<6 years) or late-onset (≥6 years). Demographic features, clinical manifestations, laboratory findings, treatments, and fulfillment of ISG, ICBD, and PEDBD criteria were evaluated. Statistical analyses included Mann-Whitney U, χ2, Fisher’s exact tests, and Spearman correlation.

RESULTS: Early-onset patients had younger symptom onset but a diagnostic delay similar to late-onset cases. Clinical manifestations, laboratory findings, and treatment approaches were comparable between groups. ISG, ICBD, and PEDBD scores showed no differences and demonstrated strong inter-correlations. Mucocutaneous features-including genital ulcers, oral aphthae, and skin lesions-were significantly less common in ICBD-negative patients, while PEDBD positivity corresponded to mucocutaneous-dominant phenotypes. CNS and vascular involvement frequently co-occurred and were associated with fewer mucocutaneous findings. None met ISG, and only one-third met ICBD, indicating limited sensitivity of current criteria for systemic-dominant presentations. No significant associations were found for ocular, joint, or febrile symptoms, and multivariate analysis was not feasible due to small subgroup sizes.

CONCLUSION: Early-onset BD shows similar clinical profiles to later-onset disease despite a tendency toward longer diagnostic delay. Current criteria insufficiently detect neurologic and vascular phenotypes, underscoring the need for pediatric-specific revisions and validation in larger cohorts.

PMID:41317363 | DOI:10.1093/rheumatology/keaf637