Author:
Sun Zhiyong,Lou Yutao,Hu Xiaoping,Song Feifeng,Zheng Xiaowei,Hu Ying,Ding Haiying,Zhang Yiwen,Huang Ping
Abstract
Abstract
Background
Radiotherapy is an essential treatment for chest cancer. Radiation-induced pulmonary fibrosis (RIPF) is an almost irreversible interstitial lung disease; however, its pathogenesis remains unclear.
Methods
We analyzed specific changes in cell populations and potential markers by using single-cell sequencing datasets from the Sequence Read Archive database, PERFORMED from control (0 Gy) and thoracic irradiated (20 Gy) mouse lungs at day 150 post-radiation. We performed IHC and ELISA on lung tissue and cells to validate the potential marker cytokines identified by the analysis on rat thoracic irradiated molds (30 Gy).
Results
Single-cell sequencing analysis showed changes in abundance across cell types and at the single-cell level, with B and T cells showing the most significant changes in abundance. And four cytokines, CCL5, ICAM1, PF4, and TNF, were significantly upregulated in lung tissues of RIPF rats and cell supernatants after ionizing radiation.
Conclusion
Cytokines CCL5, ICAM1, PF4, and TNF may play essential roles in radiation pulmonary fibrosis. They are potential targets for the treatment of radiation pulmonary fibrosis.
Funder
National Natural Science Foundation of China
Zhejiang Provincial Natural Science Foundation of China
Chinese Medicine Research Program of Zhejiang Province
Medical and Health Research Program of Zhejiang Province
Zhejiang Provincial Program for the Cultivation of New Heath Talents to Yiwen Zhang
"10000 Talents Plan" of Zhejiang Province to Ping Huang
Publisher
Springer Science and Business Media LLC
Subject
Pulmonary and Respiratory Medicine
Cited by
1 articles.
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