Radiation-induced lymphopenia does not impact treatment efficacy in a mouse tumor model

•Radiation-induce lymphopenia (RIL) is an emerging prognostic and potentially predictive factor in radioimmunotherapy.•A novel mouse model of RIL is developed and characterized in detail.•We investigate the impact of image-guided irradiation with increasing, treatment-planning-based radiotherapy tre...

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Veröffentlicht in:Neoplasia (New York, N.Y.) N.Y.), 2022-09, Vol.31, p.100812-100812, Article 100812
Hauptverfasser: Telarovic, Irma, Yong, Carmen S.M., Guckenberger, Matthias, Unkelbach, Jan, Pruschy, Martin
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Sprache:eng
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Zusammenfassung:•Radiation-induce lymphopenia (RIL) is an emerging prognostic and potentially predictive factor in radioimmunotherapy.•A novel mouse model of RIL is developed and characterized in detail.•We investigate the impact of image-guided irradiation with increasing, treatment-planning-based radiotherapy treatment volumes on the lymphocytes of healthy and tumor-bearing mice.•The impact of RIL and draining-lymph node irradiation on the treatment response to radio(immuno)therapy highly depends on the context. Radiation-induced lymphopenia is a common occurrence in radiation oncology and an established negative prognostic factor, however the mechanisms underlying the relationship between lymphopenia and inferior survival remain elusive. The relevance of lymphocyte co-irradiation as critical normal tissue component at risk is an emerging topic of high clinical relevance, even more so in the context of potentially synergistic radiotherapy-immunotherapy combinations. The impact of the radiotherapy treatment volume on the lymphocytes of healthy and tumor-bearing mice was investigated in a novel mouse model of radiation-induced lymphopenia. Using an image-guided small-animal radiotherapy treatment platform, translationally relevant tumor-oriented volumes of irradiation with an anatomically defined increasing amount of normal tissue were irradiated, with a focus on the circulating blood and lymph nodes. In healthy mice, the influence of irradiation with increasing radiotherapy treatment volumes was quantified on the level of circulating blood cells and in the spleen. A significant decrease in the lymphocytes was observed in response to irradiation, including the minimally irradiated putative tumor area. The extent of lymphopenia correlated with the increasing volumes of irradiation. In tumor-bearing mice, differential radiotherapy treatment volumes did not influence the overall therapeutic response to radiotherapy alone. Intriguingly, an improved treatment efficacy in mice treated with draining-lymph node co-irradiation was observed in combination with an immune checkpoint inhibitor. Taken together, our study reveals compelling data on the importance of radiotherapy treatment volume in the context of lymphocytes as critical components of normal tissue co-irradiation and highlights emerging challenges at the interface of radiotherapy and immunotherapy.
ISSN:1476-5586
1522-8002
1476-5586
DOI:10.1016/j.neo.2022.100812