David J Einstein, Brian Halbert, Thomas Denize, Sayed Matar, Destiny J West, Mamta Gupta, Emanuelle Andrianopoulos, Virginia Seery, Courtney Herman, Kenneth Onimus, Adrian Wells, Brittany Bunch, Sabina Signoretti, Arvind Natarajan, Anand Veerapathran, David F McDermott
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Resected primary and metastatic RCC samples were processed using the Gen 2 manufacturing process comprising of pre-Rapid Expansion Protocol (pre-REP) and REP steps. We assessed REP TILs for viability and performed phenotypic and functional characterization. We correlated the tumor immune microenvironment (TIME) with successful TIL expansion. Eight of 11 RCC samples underwent successful REP. Three failed cases demonstrated low CD8/FoxP3 ratio and high expression of PD-1 within FoxP3 cells. Expression of exhaustion markers differed between the TIME and expanded TILs; the latter had a TIM3-high/PD-1-low phenotype but retained functional capacity comparable to lifileucel. The Gen 2 manufacturing process used for lifileucel successfully expanded functional TILs from RCC samples, enabling further study in a clinical trial. 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引用次数: 0
摘要
自体治疗性肿瘤浸润淋巴细胞(TIL)疗法是一种很有前景的增强抗肿瘤免疫力的策略。优化体内外TIL扩增可扩大目前的免疫疗法选择。以前在肾细胞癌(RCC)中生成 TIL 的尝试在技术上具有挑战性。我们在 RCC 中应用了目前用于生成黑色素瘤 TIL 产品 lifileucel 的第二代生产工艺。切除的原发性和转移性RCC样本采用第二代生产工艺进行处理,该工艺包括快速扩增前协议(pre-REP)和REP步骤。我们评估了 REP TILs 的存活率,并进行了表型和功能表征。我们将肿瘤免疫微环境(TIME)与 TIL 的成功扩增联系起来。11 份 RCC 样本中有 8 份成功进行了 REP。三个失败病例的 CD8/FoxP3 比率较低,FoxP3 细胞内 PD-1 表达较高。TIME和扩增的TIL的衰竭标志物表达不同;后者的表型为TIM3-高/PD-1-低,但保留了与lifileucel相当的功能能力。用于lifileucel的第2代生产工艺成功地从RCC样本中扩增出了功能性TIL,从而可以在临床试验中进行进一步研究。CD8/FoxP3比率低和FoxP3细胞中PD-1表达高等TIME特征值得作为TIL成功扩增的潜在生物标志物进行研究。
Generation and Characterization of Ex Vivo Expanded Tumor-infiltrating Lymphocytes From Renal Cell Carcinoma Tumors for Adoptive Cell Therapy.
Autologous therapeutic tumor-infiltrating lymphocyte (TIL) therapy is a promising strategy to enhance antitumor immunity. Optimization of ex vivo TIL expansion could expand current immunotherapy options. Previous attempts to generate TIL in renal cell carcinoma (RCC) have been technically challenging. We applied a second-generation manufacturing process, currently used to generate the melanoma TIL product lifileucel, in RCC. Resected primary and metastatic RCC samples were processed using the Gen 2 manufacturing process comprising of pre-Rapid Expansion Protocol (pre-REP) and REP steps. We assessed REP TILs for viability and performed phenotypic and functional characterization. We correlated the tumor immune microenvironment (TIME) with successful TIL expansion. Eight of 11 RCC samples underwent successful REP. Three failed cases demonstrated low CD8/FoxP3 ratio and high expression of PD-1 within FoxP3 cells. Expression of exhaustion markers differed between the TIME and expanded TILs; the latter had a TIM3-high/PD-1-low phenotype but retained functional capacity comparable to lifileucel. The Gen 2 manufacturing process used for lifileucel successfully expanded functional TILs from RCC samples, enabling further study in a clinical trial. TIME features such as low CD8/FoxP3 ratio and high PD-1 expression within FoxP3 cells warrant study as potential biomarkers of successful TIL expansion.
期刊介绍:
Journal of Immunotherapy features rapid publication of articles on immunomodulators, lymphokines, antibodies, cells, and cell products in cancer biology and therapy. Laboratory and preclinical studies, as well as investigative clinical reports, are presented. The journal emphasizes basic mechanisms and methods for the rapid transfer of technology from the laboratory to the clinic. JIT contains full-length articles, review articles, and short communications.