What question did this study set out to answer?

The aim is to explore Treg dynamics and miRNA-associated differentiation mechanisms in radiation-induced lung injury.

April 17, 2026Open Access

Machine learning identifies a predictive miRNA signature and reveals the METTL3/miR-223-3p/Lif axis in regulatory T cell differentiation in radiation-induced lung injury

Key Points

The aim is to explore Treg dynamics and miRNA-associated differentiation mechanisms in radiation-induced lung injury.
Analyzed Treg changes in irradiated mouse lungs using single-cell RNA sequencing and flow cytometry.
Evaluated Treg roles in neutrophil and monocyte infiltration via anti-CD25 antibodies.
Identified miRNA/mRNA signatures with high-throughput sequencing and validated using plasma profiles.
Constructed a predictive model using machine learning methods like JMI and SVM-RFE.
Found that miR-223-3p directly targets Lif to regulate Treg differentiation.
METTL3 inhibits miR-223-3p maturation via m6A modification, thereby reducing Treg accumulation in lung injury.
Achieved a predictive model with high accuracy, indicated by an AUC of 0.997.

Abstract

This study examined regulatory T cell (Treg) dynamics in radiation-induced lung injury (RILI), focusing on miRNA/mRNA-mediated differentiation mechanisms to identify therapeutic targets. Temporal Treg changes in irradiated mouse lungs were analyzed via single-cell RNA sequencing (scRNA-seq) and flow cytometry. Treg ablation via anti-CD25 antibodies assessed their regulatory roles in neutrophil and monocyte infiltration. High-throughput sequencing identified miRNAs/mRNAs governing Treg differentiation. Plasma miRNA profiles from GSE147242 were enrolled to validate the differential expression of miR-223-3p in RILI. Additionally, machine learning methods were used to construct most predictive miRNA signature post- radiotherapy alterations. Dual-luciferase assays validated miR-223-3p binding to leukemia inhibitory factor (Lif). In vivo/in vitro experiments evaluated METTL3’s impact on miR-223-3p maturation and Treg differentiation. Treg infiltration increased in RILI and bleomycin-induced fibrosis, interacting with epithelial, endothelial, and fibroblast cells. miR-223-3p directly targeted Lif to regulate Treg differentiation, while METTL3 suppressed miR-223-3p maturation via m6A modification. METTL3 inhibition reduced Treg accumulation and alleviated lung injury. Additionally, plasma miRNA analysis confirmed marked differential expression of miR-223-3p post-radiotherapy. A predictive model, integrating miR-223-3p, miR-150-5p, and miR-34a-5p via JMI and SVM-RFE machine learning methods, achieved an AUC of 0.997 (five-fold cross-validation AUC: 0.973), highlighting its high predictive efficacy. scRNA-seq revealed resting Tregs differentiating into Th2-like subsets (marked by KLRG1 and GATA3) with altered m6A levels, implicating epitranscriptional control of Treg plasticity. Tregs mediate multicellular interactions in irradiated lungs. METTL3 promotes miR-223-3p maturation via m6A and drives Treg differentiation through Lif. The METTL3/miR-223-3p/Lif axis regulates Treg-mediated fibrosis, highlighting METTL3 as a therapeutic target for RILI.

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Peng et al. (Wed,) studied this question.

synapsesocial.com/papers/69e1ceaa5cdc762e9d857a5d https://doi.org/https://doi.org/10.1016/j.gendis.2026.102186

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