Doxorubicin enhances the abscopal effect depending on tumor cell mitochondrial DNA and STING
MO-0726
Abstract
Doxorubicin enhances the abscopal effect depending on tumor cell mitochondrial DNA and STING
Authors: Liqun Wang1, Ren Luo2, Kateryna Onyshchenko3, Gabriele Niedermann4
1University of Freiburg, Department of Radiation Oncology, Freiburg, Germany; 2Department of Thoracic Oncology Ward, Cancer Center and State Key Laboratory of Biotherapy, West China Hospital, Chengdu, China; 3Department of Radiation Oncology, University of Freiburg, Freiburg, Germany; 4 Department of Radiation Oncology, University of Freiburg , Freiburg , Germany
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Purpose or Objective
Localized radiotherapy (RT) can cause a T cell-mediated abscopal effect on non-irradiated tumor lesions, especially in combination with immune checkpoint blockade (ICB). However, this effect is still clinically rare and improvements are highly desirable. We investigated whether triple combination with a low dose of clinically approved liposomal doxorubicin (Doxil) could augment abscopal responses compared with RT plus ICB and Doxil plus ICB.
Material and Methods
We used Doxil in combination with RT and αPD-1 in two tumor models (B16-CD133 melanoma and MC38 colon carcinoma) with mice bearing two tumors, only one of which was irradiated.
Results
We show in these two models that triple therapy with RT, αPD-1, and single low-dose Doxil strongly enhanced the RT-induced abscopal effect. Complete cures of non-irradiated tumors were mainly observed in triple-treated mice. Triple therapy induced more cross-presenting dendritic cells (DCs) and more tumor-specific CD8+ T cells than RT/αPD-1 and Doxil/αPD-1, particularly in non-irradiated tumors. CD8+ T cell depletion or implantation of STING-deficient tumor cells abolished the abscopal effect. cGAS/STING detects cytosolic DNA, triggering type I IFN expression, which drives antitumor CD8+ T cell responses through cross-presenting DCs. To date, it is not fully understood how doxorubicin/Doxil induces type I IFN and which nucleic acid species is critical for this. By using inhibitors and knockout cells, we show that doxorubicin/Doxil-induced IFNβ1 markedly depended on the cGAS/STING pathway. In mitochondrial DNA (mtDNA)-depleted tumor cells, doxorubicin/Doxil induced less secretion of IFNβ1, the related T cell-recruiting chemokine CXCL10, and ATP; coincubation with mtDNA-depleted tumor cells strongly reduced IFNβ1 secretion by DCs. Implantation of mtDNA-depleted tumor cells, particularly at the non-irradiated/abscopal site, substantially diminished the Doxil-enhanced abscopal effect and tumor infiltration by tumor-specific CD8+ T cells.
Conclusion
These data show that single low-dose Doxil can substantially enhance the RT-induced abscopal effect, with a strong increase in cross-presenting DCs and CD8+ tumor-specific T cells particularly in abscopal tumors compared with RT/αPD-1 and Doxil/αPD-1. Moreover, they indicate that the mtDNA/cGAS/STING/IFN-I axis is important for the immunogenic doxorubicin effects. Our findings may be helpful for the planning of clinical radiochemoimmunotherapy trials in (oligo)metastatic patients.