An attenuated lymphocytic choriomeningitis virus vector enhances tumor control in mice partly via IFN-I
Young Rock Chung, … , Slim Fourati, Pablo Penaloza-MacMaster
Young Rock Chung, … , Slim Fourati, Pablo Penaloza-MacMaster
Published June 11, 2024
Citation Information: J Clin Invest. 2024;134(15):e178945. https://doi.org/10.1172/JCI178945.
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An attenuated lymphocytic choriomeningitis virus vector enhances tumor control in mice partly via IFN-I

Abstract

Viral vectors are being used for the treatment of cancer. Yet, their efficacy varies among tumors and their use poses challenges in immunosuppressed patients, underscoring the need for alternatives. We report striking antitumoral effects by a nonlytic viral vector based on attenuated lymphocytic choriomeningitis virus (r3LCMV). We show in multiple tumor models that injection of tumor-bearing mice with this vector results in improved tumor control and survival. Importantly, r3LCMV improved tumor control in immunodeficient Rag1–/– mice and MyD88–/– mice, suggesting that multiple pathways contributed to the antitumoral effects. The antitumoral effects of r3LCMV were also observed when this vector was administered several weeks before tumor challenges, suggesting the induction of trained immunity. Single-cell RNA sequencing analyses, antibody blockade experiments, and knockout models revealed a critical role for host-intrinsic IFN-I in the antitumoral efficacy of r3LCMV vectors. Collectively, these data demonstrate potent antitumoral effects by r3LCMV vectors and unveil multiple mechanisms underlying their antitumoral efficacy.

Authors

Young Rock Chung, Bakare Awakoaiye, Tanushree Dangi, Nahid Irani, Slim Fourati, Pablo Penaloza-MacMaster

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Figure 4

r3LCMV therapy improves tumor control in Rag1–/– mice.

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r3LCMV therapy improves tumor control in Rag1–/– mice. (A) Experiment ou...
(A) Experiment outline. (B) Tumor control. (C) Survival. (D) Viral loads in tumors at day 21 after treatment. Viral loads were quantified by plaque assays on Vero cell monolayers. Data from B and C are pooled from 2 experiments (one experiment with n = 5 per group and another with n = 5–9 per group). Data from D are from the tumors of 7 Rag1–/– mice that were treated with r3LCMV and survived until day 21 (tumors of 10 wild-type mice that were treated with r3LCMV and survived until day 21 are included for comparison). Error bars represent SEM. Indicated P values were calculated by the Mann-Whitney test, or log rank test when comparing survival.