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Overcome the challenge for intratumoral injection of STING agonist for pancreatic cancer by systemic administration

医学 胰腺癌 血液学 全身给药 兴奋剂 癌症 遗产管理(遗嘱认证法) 内科学 肿瘤科 受体 生物 航空航天工程 生物技术 法学 体内 工程类 政治学
作者
Keyu Li,Junke Wang,Rui Zhang,Jiawei Zhou,Birginia Espinoza,Nan Niu,Jianxin Wang,Noelle R. Jurcak,Noah Rozich,Arsen Osipov,MacKenzie Henderson,Vanessa Funes,Melissa R. Lyman,Alex B. Blair,Brian Herbst,Mengni He,Jialong Yuan,Diego Trafton,Chunhui Yuan,Michael Wichroski
出处
期刊:Journal of Hematology & Oncology [BioMed Central]
卷期号:17 (1) 被引量:7
标识
DOI:10.1186/s13045-024-01576-z
摘要

Due to the challenge for intratumoral administration, innate agonists have not made it beyond preclinical studies for efficacy testing in most tumor types. Pancreatic ductal adenocarcinoma (PDAC) has a hostile tumor microenvironment that renders T cells dysfunctional. Innate agonist treatments may serve as a T cell priming mechanism to sensitize PDACs to anti-PD-1 antibody (a-PD-1) treatment. Using a transplant mouse model with spontaneously formed liver metastasis, a genetically engineered KPC mouse model that spontaneously develops PDAC, and a human patient-derived xenograft model, we compared the antitumor efficacy between intrahepatic/intratumoral and intramuscular systemic administration of BMS-986301, a next-generation STING agonist. Flow cytometry, Nanostring, and cytokine assays were used to evaluate local and systemic immune responses. This study demonstrated that administration of STING agonist systemically via intramuscular injection is equivalent to its intratumoral injection in inducing both effector T cell response and antitumor efficacy. Compared to intratumoral administration, T cell exhaustion and immunosuppressive signals induced by systemic administration were attenuated. Nonetheless, either intratumoral or systemic treatment of STING agonist was associated with increased expression of CTLA-4 on tumor-infiltrating T cells. However, the combination of a-PD-1 and anti-CTLA-4 antibody with systemic STING agonist demonstrated the antitumor efficacy in the KPC mouse spontaneous PDAC model. The mouse pancreatic and liver orthotopic model of human patient-derived xenograft reconstituted with PBMC also showed that antitumor and abscopal effects of both intratumoral and intramuscular STING agonist are equivalent. Taken together, this study supports the clinical development of innate agonists via systemic administration for treating PDAC.
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