FLASH Irradiation Spares Lung Progenitor Cells and Limits the Incidence of Radio-induced Senescence

祖细胞 衰老 闪光灯(摄影) 生物 入射(几何) 癌症研究 祖细胞 辐照 医学 病理 干细胞 细胞生物学 内科学 物理 光学 核物理学
作者
Charles Fouillade,Sandra Curras-Alonso,Lorena Giuranno,Eddy Quelennec,Sophie Heinrich,Sarah Bonnet-Boissinot,Arnaud Beddok,Sophie Leboucher,Hamza Umut Karakurt,Mylène Bohec,Sylvain Baulande,Marc Vooijs,Pierre Verrelle,Marie Dutreix,Arturo Londoño‐Vallejo,Vincent Favaudon
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:26 (6): 1497-1506 被引量:230
标识
DOI:10.1158/1078-0432.ccr-19-1440
摘要

Abstract Purpose: One of the main limitations to anticancer radiotherapy lies in irreversible damage to healthy tissues located within the radiation field. “FLASH” irradiation at very high dose-rate is a new treatment modality that has been reported to specifically spare normal tissue from late radiation-induced toxicity in animal models and therefore could be a promising strategy to reduce treatment toxicity. Experimental Design: Lung responses to FLASH irradiation were investigated by qPCR, single-cell RNA sequencing (sc-RNA-Seq), and histologic methods during the acute wound healing phase as well as at late stages using C57BL/6J wild-type and Terc−/− mice exposed to bilateral thorax irradiation as well as human lung cells grown in vitro. Results: In vitro studies gave evidence of a reduced level of DNA damage and induced lethality at the advantage of FLASH. In mouse lung, sc-RNA-seq and the monitoring of proliferating cells revealed that FLASH minimized the induction of proinflammatory genes and reduced the proliferation of progenitor cells after injury. At late stages, FLASH-irradiated lungs presented less persistent DNA damage and senescent cells than after CONV exposure, suggesting a higher potential for lung regeneration with FLASH. Consistent with this hypothesis, the beneficial effect of FLASH was lost in Terc−/− mice harboring critically short telomeres and lack of telomerase activity. Conclusions: The results suggest that, compared with conventional radiotherapy, FLASH minimizes DNA damage in normal cells, spares lung progenitor cells from excessive damage, and reduces the risk of replicative senescence.
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