摘要:溶瘤病毒衍生的I型干扰素与EGFRvIII CAR - t细胞之间的意外拮抗作用

Genetically Engineered T-cells Pub Date : 2019-02-01 DOI:10.1158/2326-6074.CRICIMTEATIAACR18-A029

Laura Evgin, Amanda L. Huff, Phonphimon Wongthida, Jill Thompson, T. Kottke, J. Sampson, L. Perez, R. Vile

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引用次数: 0

摘要

尽管嵌合抗原受体(CAR) t细胞平台在血液系统恶性肿瘤患者中取得了临床成功，但针对实体肿瘤靶点的CAR - t细胞的疗效有限。溶瘤病毒的高度炎症性质及其重塑肿瘤微环境的能力向我们表明，它们将提供一种互补的作用机制，以招募和增强CAR - t细胞的功能。将VSVmIFNβ注射到B16EGFRvIII肿瘤中增加了趋化因子如CXCL10和CCL5的表达，我们预计这些趋化因子会募集CXCR3+和CCR5+ EGFRvIII特异性小鼠CAR - t细胞。然而，与CAR - t细胞单药治疗相比，我们没有观察到使用联合策略的总生存期或肿瘤控制的增加。我们在过继转移后早期从注射了VSVmIFNβ的肿瘤中回收了较少的活CD8+ CAR - t细胞，并观察到在血液中长期存在的CD8+ CAR - t细胞数量的类似减少。我们已经证明，I型干扰素增加了来自逆转录病毒LTR的CAR的表达，并反过来使这些细胞对滋补信号介导的衰竭和凋亡敏感。相应地，IFNAR KO t细胞制备的CAR - t细胞在体内可以免受I型IFN的有害作用。我们目前正在研究克服这两种模式之间干扰的策略，并从I型IFN信号中解耦CAR表达的调节。引文格式:Laura Evgin, Amanda L. Huff, Phonphimon Wongthida, Jill Thompson, Timothy Kottke, John Sampson, Luis Sanchez Perez, Richard Vile。溶瘤病毒衍生的I型干扰素与EGFRvIII CAR - t细胞之间的意外拮抗作用[摘要]。第四届CRI-CIMT-EATI-AACR国际癌症免疫治疗会议:将科学转化为生存;2018年9月30日至10月3日;纽约，纽约。费城(PA): AACR;癌症免疫学杂志2019;7(2增刊):摘要nr A029。

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Abstract A029: Unexpected antagonism between oncolytic virus derived type I interferon and EGFRvIII CAR T-cells

Although the chimeric antigen receptor (CAR) T-cell platform has experienced clinical success in patients with hematologic malignancies, CAR T-cells specific to solid tumor targets have met with more limited efficacy. The highly inflammatory nature of oncolytic viruses and their ability to remodel the tumor microenvironment suggested to us that they would provide a complementary mechanism of action to both recruit and potentiate the functionality of CAR T-cells. VSVmIFNβ injection into B16EGFRvIII tumors increased the expression of chemokines such as CXCL10 and CCL5, which we would expect to recruit CXCR3+and CCR5+ EGFRvIII specific murine CAR T-cells. However, we did not observe an increase in overall survival or tumor control using the combination strategy compared to monotherapy with CAR T-cells. We recovered fewer viable CD8+ CAR T-cells from tumors injected with VSVmIFNβ early after adoptive transfer, and observed a similar reduction in the number of CD8+ CAR T-cells which persisted long term in the blood. We have shown that type I interferon increases the expression of the CAR from the retroviral LTR and in turn sensitizes these cells to tonic signaling mediated exhaustion and apoptosis. Correspondingly, CAR T-cells prepared from IFNAR KO T-cells were protected from the deleterious effect of type I IFN in vivo. We are currently investigating strategies to overcome the interference between these two modalities and to uncouple the regulation of the expression of the CAR from type I IFN signaling. Citation Format: Laura Evgin, Amanda L. Huff, Phonphimon Wongthida, Jill Thompson, Timothy Kottke, John Sampson, Luis Sanchez Perez, Richard Vile. Unexpected antagonism between oncolytic virus derived type I interferon and EGFRvIII CAR T-cells [abstract]. In: Proceedings of the Fourth CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; Sept 30-Oct 3, 2018; New York, NY. Philadelphia (PA): AACR; Cancer Immunol Res 2019;7(2 Suppl):Abstract nr A029.

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Genetically Engineered T-cells

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