IL-36γ and the Development and Validation of an Early Prediction Model for Severe Mycoplasma Pneumoniae Pneumonia in Children

Authors

XiaoDong Tang, Department of Pediatric, Suzhou Hospital of AnHui Medical University, SuZhou, China
Ying Li, Department of Pediatric, Suzhou Hospital of AnHui Medical University, SuZhou, China
Pao Yu, Department of Pediatric, Suzhou Hospital of AnHui Medical University, SuZhou, China
WenPeng Wang, Department of Pediatrics, The Affiliated Hospital of Xuzhou Medical University, XuZhou, China
Bi Zhou, Department of Pediatric, Suzhou Hospital of AnHui Medical University, SuZhou, ChinaFollow

Abstract

Objective: This study aimed to retrospectively analyze clinical data from pediatric patients with Mycoplasma pneumoniae pneumonia (MPP), investigate the expression and clinical significance of serum IL-36γ, and to develop and validate an early identification model for severe MPP (SMPP). Methods: Clinical data were collected from 345 children diagnosed with MPP in our department between July 1, 2023, and December 31, 2024. Based on diagnostic criteria, enrolled patients were categorized into an SMPP group (n=145) and a non-severe MPP (NSMPP) group (n=200). Serum IL-36γ levels at admission were measured using ELISA. Independent risk factors for SMPP were identified via binary logistic regression, and a nomogram prediction model was constructed. An external validation cohort consisted of clinical data from 148 MPP patients (61 SMPP, 87 NSMPP) treated concurrently in the Xuzhou Medical University Affiliated Hospital. The model was evaluated using ROC curves, calibration curves, and decision curve analysis (DCA). Results: Age, ESR, albumin, hsCRP, and IL-36γ may serve as independent factors for the early identification of children with SMPP. Based on these five indicators, a nomogram prediction model was developed. ROC curve analysis showed an area under the curve (AUC) of 0.89 in the training set (accuracy = 0.81, sensitivity = 0.78, specificity = 0.84), and an AUC of 0.89 in the validation set (accuracy = 0.83, sensitivity = 0.80, specificity = 0.87). Calibration curves indicated good model fit in both the training and validation sets. Furthermore, decision curve analysis (DCA) suggested that the model demonstrates potential clinical applicability across a range of threshold probabilities. Conclusion: This study developed a nomogram model that showed promising predictive performance for the early identification of pediatric SMPP. Following internal and external validation, our findings suggest that this model could potentially serve as a decision-support tool to aid in risk stratification and guide timely clinical intervention, though further prospective studies are warranted to confirm its utility.

Recommended Citation

Tang, XiaoDong; Li, Ying; Yu, Pao; Wang, WenPeng; and Zhou, Bi (2026) "IL-36γ and the Development and Validation of an Early Prediction Model for Severe Mycoplasma Pneumoniae Pneumonia in Children," Journal of Pediatric Infectious Diseases: Vol. 21: Iss. 1, Article 6.
DOI: https://doi.org/10.53391/1305-7707.1055
Available at: https://jpid.researchcommons.org/journal/vol21/iss1/6