Immunotherapy enhances the risk of tumor oxidative stress and metastasis in lung cancer with radiation pneumonitis
Ruidi Jiao, Wenbo Xu, Kunpeng Xu, Mingxia Zhang, Weilong Liu, Wei Jiang, Luhua Wang

TL;DR
This study shows that radiation pneumonitis worsens lung cancer immunotherapy outcomes by increasing oxidative stress and metastasis.
Contribution
The paper reveals a novel RP-ICB-metabolism axis linking radiation pneumonitis to immunotherapy resistance through oxidative stress and immune microenvironment changes.
Findings
Immunotherapy combined with RP increases liver metastasis and neutrophil infiltration in lung cancer.
RP and immunotherapy synergistically cause lipid metabolic dysregulation and oxidative stress.
Higher oxidative stress scores correlate with poor immunotherapy response and worse clinical outcomes.
Abstract
Radiation pneumonitis (RP) is a prevalent complication associated with lung cancer radiotherapy; nonetheless, its effects on lung cancer immunotherapy and the underlying biological mechanisms remain inadequately elucidated. Utilizing mouse models of RP and orthotopically lung cancer, we witnessed immunotherapy-enhanced liver metastasis of lung cancer within the context of RP, accompanied by increased neutrophil infiltration of the primary tumor. Analysis of metabolic adaptations driven by the inflammatory microenvironment during treatment revealed that RP and immunotherapy act synergistically to exacerbate lipid metabolic dysregulation and oxidative stress. Integrating clinical validation with single-cell RNA sequencing data from a multicenter lung adenocarcinoma cohort, we demonstrated that elevated oxidative stress scores within tumor tissue were significantly associated with both…
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Taxonomy
TopicsCancer Immunotherapy and Biomarkers · Immune cells in cancer · Ferroptosis and cancer prognosis
