Assessing Longitudinal Treatment Efficacies and Alterations in Molecular Markers Associated with Glutamatergic Signaling and Immune Checkpoint Inhibitors in a Spontaneous Melanoma Mouse Model

Kevinn Eddy , Kajal Gupta , Mohamad Naser Eddin , Christina Marinaro , Sanjana Putta , John Michael Sauer Jr , Anna Chaly , Katie B. Freeman , Jeffrey C. Pelletier , Anna Fateeva , Philip Furmanski , Ann W. Silk , Allen B. Reitz , Andrew Zloza , Suzie Chen
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Abstract

Previous work done by our laboratory described the use of an immunocompetent spontaneous melanoma-prone mouse model, TGS (TG-3/SKH-1), to evaluate treatment outcomes using inhibitors of glutamatergic signaling and immune checkpoint for 18 weeks. We showed a significant therapeutic efficacy with a notable sex-biased response in male mice. In this follow-up 18-week study, the dose of the glutamatergic signaling inhibitor was increased (from 1.7 mg/kg to 25 mg/kg), which resulted in improved responses in female mice but not male mice. The greatest reduction in tumor progression was observed in male mice treated with single-agent troriluzole and anti–PD-1. Furthermore, a randomly selected group of mice was removed from treatment after 18 weeks and maintained for up to an additional 48 weeks demonstrating the utility of the TGS mouse model to perform a ≥1-year preclinical therapeutic study in a physiologically relevant tumor–host environment. Digital spatial imaging analyses were performed in tumors and tumor microenvironments across treatment modalities using antibody panels for immune cell types and immune cell activation. The results suggest that immune cell populations and cytotoxic activities of T cells play critical roles in treatment responses in these mice. Examination of a group of molecular protein markers based on the proposed mechanisms of action of inhibitors of glutamatergic signaling and immune checkpoint showed that alterations in expression levels of xCT, γ-H2AX, EAAT2, PD-L1, and PD-1 are likely associated with the loss of treatment responses. These results suggest the importance of tracking changes in molecular markers associated with the mechanism of action of therapeutics over the course of a longitudinal preclinical therapeutic study in spatial and temporal manners.

评估自发性黑色素瘤小鼠模型的纵向治疗效果以及与谷氨酸信号传导和免疫检查点抑制剂相关的分子标记物的变化
我们实验室之前的工作描述了使用免疫功能正常的自发性黑色素瘤易感小鼠模型 TGS(TG-3/SKH-1)来评估使用谷氨酸能信号传导抑制剂和免疫检查点进行为期 18 周的治疗效果。结果表明,雄性小鼠的疗效显著,且具有明显的性别差异。在这项为期18周的后续研究中,我们增加了谷氨酸信号转导抑制剂的剂量(从1.7毫克/千克增加到25毫克/千克),结果雌性小鼠的反应有所改善,而雄性小鼠则没有。雄性小鼠在接受单药曲利鲁唑和抗-PD-1治疗后,肿瘤进展的减少幅度最大。此外,随机选取的一组小鼠在治疗18周后脱离治疗,并继续维持48周,这表明TGS小鼠模型可以在生理相关的肿瘤-宿主环境中进行为期≥1年的临床前治疗研究。使用免疫细胞类型和免疫细胞活化抗体板对不同治疗模式下的肿瘤和肿瘤微环境进行了数字空间成像分析。结果表明,免疫细胞群和 T 细胞的细胞毒活性在这些小鼠的治疗反应中起着关键作用。根据谷氨酸能信号传导抑制剂和免疫检查点抑制剂的作用机制对一组分子蛋白标记物进行的研究表明,xCT、γ-H2AX、EAAT2、PD-L1 和 PD-1 表达水平的改变可能与治疗反应的丧失有关。这些结果表明,在纵向临床前治疗研究过程中,以空间和时间方式跟踪与治疗药物作用机制相关的分子标记物的变化非常重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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