Tumor Treating Fields dually activate STING and AIM2 inflammasomes to induce adjuvant immunity in glioblastoma
Dongjiang Chen, … , Maryam Rahman, David D. Tran
Dongjiang Chen, … , Maryam Rahman, David D. Tran
Published February 24, 2022
Citation Information: J Clin Invest. 2022;132(8):e149258. https://doi.org/10.1172/JCI149258.
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Research Article Oncology

Tumor Treating Fields dually activate STING and AIM2 inflammasomes to induce adjuvant immunity in glioblastoma

Abstract

Tumor Treating Fields (TTFields), an approved therapy for glioblastoma (GBM) and malignant mesothelioma, employ noninvasive application of low-intensity, intermediate-frequency, alternating electric fields to disrupt the mitotic spindle, leading to chromosome missegregation and apoptosis. Emerging evidence suggests that TTFields may also induce inflammation. However, the mechanism underlying this property and whether it can be harnessed therapeutically are unclear. Here, we report that TTFields induced focal disruption of the nuclear envelope, leading to cytosolic release of large micronuclei clusters that intensely recruited and activated 2 major DNA sensors — cyclic GMP-AMP synthase (cGAS) and absent in melanoma 2 (AIM2) — and their cognate cGAS/stimulator of interferon genes (STING) and AIM2/caspase 1 inflammasomes to produce proinflammatory cytokines, type 1 interferons (T1IFNs), and T1IFN-responsive genes. In syngeneic murine GBM models, TTFields-treated GBM cells induced antitumor memory immunity and a cure rate of 42% to 66% in a STING- and AIM2-dependent manner. Using single-cell and bulk RNA sequencing of peripheral blood mononuclear cells, we detected robust post-TTFields activation of adaptive immunity in patients with GBM via a T1IFN-based trajectory and identified a gene panel signature of TTFields effects on T cell activation and clonal expansion. Collectively, these studies defined a therapeutic strategy using TTFields as cancer immunotherapy in GBM and potentially other solid tumors.

Authors

Dongjiang Chen, Son B. Le, Tarun E. Hutchinson, Anda-Alexandra Calinescu, Mathew Sebastian, Dan Jin, Tianyi Liu, Ashley Ghiaseddin, Maryam Rahman, David D. Tran

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Figure 8

Induction of antitumor immunity in the GL261 syngeneic GBM model by TTFields requires STING and AIM2.

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Induction of antitumor immunity in the GL261 syngeneic GBM model by TTFi...
(See Supplemental Figures 12–15). Antitumor immunity in C57BL/6J mice induced by TTFields-treated GL261-luc GBM cells. Representative photographs showing orthotopic GBM tumor growth by BLI after immunization with Scr/NT (n = 9), Scr/TTF (n = 12), DKD/NT (n = 9), or DKD/TTF (n = 10) cells (A) and after rechallenge with twice the number of parental cells in the surviving Scr/TTF cohort (n = 5) and a new naive cohort (n = 12) (B). (C) Kaplan-Meier estimates showing survival rates after initial immunization and rechallenge and the immune TME summarized with a heatmap of a 29-immune gene expression profile by qRT-PCR (n = 5 per cohort) (D) and representative images of IF for CD8, CD3, and DAPI counterstain (E). Scale bar: 50 μm. Log-rank test was used to compare survival rates and 2-way ANOVA to compare immune TME profile differences. ***P < 0.001. NS, not significant.