Immune targeting of triple-negative breast cancer through a clinically actionable STING agonist-CAR T cell platform.

IF 11.7 1区医学 Q1 CELL BIOLOGY

Cell Reports Medicine Pub Date : 2025-06-14 DOI:10.1016/j.xcrm.2025.102198

Yuqing Zhang, Zehua Li, Jessica Ritter, Elliott J Brea, Navin R Mahadevan, Deborah A Dillon, Sung-Rye Park, Eric Minwei Liu, Michael Y Tolstorukov, William E McGourty, Patrick Lizotte, Elena V Ivanova, Caroline Fahey, Koji Haratani, Tran C Thai, Kara M Soroko, Sophie Kivlehan, Eric L Smith, Prafulla C Gokhale, Cloud P Paweletz, David A Barbie, Thanh U Barbie

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引用次数: 0

Abstract

Stimulator of interferon genes (STING) has emerged as a critical cancer immunotherapy target. However, no STING agonist has advanced beyond phase I/II clinical trials, as obstacles center around applying STING agonism to the appropriate clinical context, retaining it in the tumor microenvironment (TME), and limiting its T cell toxicity. Using triple-negative breast cancer (TNBC), we identify defective STING turnover as a cancer state promoting hypersensitivity to STING agonism. We also repurpose a US Food and Drug Administration (FDA)-approved polyethylene glycol (PEG) biopsy marker to deliver STING agonists in a controlled release fashion into the TME. However, STING agonist-induced T cell toxicity limits robust endogenous clonal T cell response, which can be overcome by sequential co-delivery of the STING agonists with CAR T cell therapy using the same PEG marker, eradicating orthotopic TNBC in mouse models while also controlling distant disease. These findings identify a highly translatable platform to combine STING agonists with CAR T cell therapy locally for TNBC and potentially other solid cancers.

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通过临床可操作的STING激动剂- car - T细胞平台免疫靶向三阴性乳腺癌。

干扰素基因刺激因子（STING）已成为肿瘤免疫治疗的重要靶点。然而，没有一种STING激动剂能超过I/II期临床试验，因为障碍集中在将STING激动剂应用于适当的临床环境，将其保留在肿瘤微环境（TME）中，以及限制其T细胞毒性。使用三阴性乳腺癌（TNBC），我们确定有缺陷的STING转换是一种促进对STING激动剂过敏的癌症状态。我们还重新利用了美国食品和药物管理局（FDA）批准的聚乙二醇（PEG）活检标记物，以可控释放的方式将STING激动剂输送到TME。然而，STING激动剂诱导的T细胞毒性限制了强大的内源性克隆T细胞反应，这可以通过使用相同的PEG标记物将STING激动剂与CAR - T细胞治疗顺序共递送来克服，从而在小鼠模型中根除原位TNBC，同时控制远处疾病。这些发现确定了一个高度可翻译的平台，将STING激动剂与CAR - T细胞局部治疗TNBC和潜在的其他实体癌。

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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来源期刊

Cell Reports Medicine Biochemistry, Genetics and Molecular Biology-Biochemistry, Genetics and Molecular Biology (all)

CiteScore

15.00

自引率

1.40%

发文量

231

审稿时长

40 days

期刊介绍： Cell Reports Medicine is an esteemed open-access journal by Cell Press that publishes groundbreaking research in translational and clinical biomedical sciences, influencing human health and medicine. Our journal ensures wide visibility and accessibility, reaching scientists and clinicians across various medical disciplines. We publish original research that spans from intriguing human biology concepts to all aspects of clinical work. We encourage submissions that introduce innovative ideas, forging new paths in clinical research and practice. We also welcome studies that provide vital information, enhancing our understanding of current standards of care in diagnosis, treatment, and prognosis. This encompasses translational studies, clinical trials (including long-term follow-ups), genomics, biomarker discovery, and technological advancements that contribute to diagnostics, treatment, and healthcare. Additionally, studies based on vertebrate model organisms are within the scope of the journal, as long as they directly relate to human health and disease.