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Abstract 2224A: A novel TNFRSF25 agonist, PTX35, synergizes with Gp96-Ig/OX40L-Ig to enhance effector and memory anti-tumor CD8+ T cell responses and delay tumor growth

CD8型 T细胞 记忆T细胞 细胞毒性T细胞 癌症研究 生物 抗原 免疫学 效应器 肿瘤微环境 单克隆抗体 抗体 免疫系统 体外 生物化学
作者
Vikas Tahiliani,Patrick M. Dillon,Jayalakshmi Miriyala,Anh M. Trinh,Rahul R. Jasuja,Jeff Hutchins,Yvonne Paterson
出处
期刊:Cancer Research [American Association for Cancer Research]
卷期号:80 (16_Supplement): 2224A-2224A
标识
DOI:10.1158/1538-7445.am2020-2224a
摘要

Abstract We have developed a next generation cellular vaccine platform that incorporates a tumor antigen chaperone (gp96-Ig) in a tumor cell line and a host of over-expressed cancer associated neoantigens. Viagenpumatucel-L (HS-110), a human lung adenocarcinoma cell line, stably transfected to express gp96-Ig, is being tested in a phase 1/2 clinical trial (NCT#02439450) for NSCLC. Heat has recently developed HS-130, an allogeneic cell-based vaccine, designed to secrete tumor-associated antigens along with a costimulatory molecule, OX40L-Fc. Preclinical results of mouse HS-130 (mHS-130) in combination with mouse HS-110 (mHS-110) has shown a potent anti-tumor effector and memory CD8+ T cell response, followed by tumor regression. In our current study, we further characterized the role of mHS-110 and mHS-130 in combination with an agonist TNFRSF25 monoclonal antibody (mAb), PTX-35. PTX-35 is a potent stimulator of effector and memory CD8+ T cell responses, which taken together with HS-110 and HS130 has the potential of treating human cancers. To study expansion, contraction, and maintenance of tumor-specific CD8+ T cell responses, mHS-110 and/or mHS-130, in combination with different doses of mouse-IgG1-PTX-35 (mPTX-35) was administered to C57BL/6 mice that were adoptively transferred with syngeneic OVA-specific T cells (OT-I). Mice were then challenged with murine melanoma tumors (B16F10-OVA) to characterize the tumor-specific immune cells in the periphery, spleen, and tumor-microenvironment that were involved in tumor regression. Combination of mPTX-35 with mHS-110 and mHS-130 increased the expansion of tumor-specific CD8+ T-cells, in a mPTX-35 dose-dependent manner. This cellular expansion was significantly higher in the 1 mg/kg dose of mPTX-35 and far exceeded the additive value of mPTX-35, mHS-130, and mHS-110 treatment alone. Systemic administration of mPTX-35, in combination with mHS-110 and mHS-130, led to a significant increase in the expansion of activated CD8+ T cells in the blood and stimulated activation of effector memory CD8+ T cells residing in the spleen. Importantly, this combination resulted in higher frequencies of tumor infiltrating lymphocytes (TILs), which enhanced regression of established B16F10-OVA tumors and increased overall survival. These results strongly suggest that mPTX-35 synergizes with mHS-110 and mHS-130 to amplify activated tumor-specific CD8+ T cells, program a strong memory response, and allow for tumor regression. We also assessed if PD-1 antagonist therapies further amplified our responses and found that checkpoint inhibition (CPI) synergizes effectively with PTX-35 and mHS-110. Therefore, the combinations of these treatments along with CPI may translate into an efficacious approach to treating human cancers. Citation Format: Vikas Tahiliani, Patrick Dillon, Jayalakshmi Miriyala, Anh Trinh, Rahul R. Jasuja, Jeff Hutchins, Matthew M. Seavey. A novel TNFRSF25 agonist, PTX35, synergizes with Gp96-Ig/OX40L-Ig to enhance effector and memory anti-tumor CD8+ T cell responses and delay tumor growth [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 2224A.

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