Functional avidity of anti-B7H3 CAR-T constructs predicts antigen density thresholds for triggering effector function

IF 15.7 1区综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES

Nature Communications Pub Date : 2025-08-05 DOI:10.1038/s41467-025-61427-4

Marta Barisa, Henrike P. Muller, Elisa Zappa, Rivani Shah, Juliane L. Buhl, Benjamin Draper, Courtney Himsworth, Chantelle Bowers, Sophie Munnings-Tomes, Marilena Nicolaidou, Sonia Morlando, Kathleen Birley, Clara Leboreiro-Babe, Alice Vitali, Laura Privitera, Kyle O’Sullivan, Ailsa Greppi, Magdalena Buschhaus, Mario Barrera Román, Sam de Blank, Femke van den Ham, Brenna R. van ‘t Veld, Gabrielle Ferry, Jonathan Fisher, Debarati Shome, Reza Nadafi, Israrul H. Ansari, Rogier Reijmers, Stefano Giuliani, Paul Sondel, Laura K. Donovan, Louis Chesler, Jan Molenaar, Jarno Drost, Anne C. Rios, Kerry Chester, Judith Wienke, John Anderson

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Abstract

Chimeric Antigen receptor T cell (CAR-T) treatments for solid cancers have been compromised by limited expansion and survival in the tumor microenvironment following interaction with antigen-expressing target cells. Using B7H3 as a model antigen with broad clinical applicability, we evaluate the relationship between the antibody/antigen affinity of three clinical candidate binders and the three following characteristics: cellular avidity, duration of sustained cytotoxicity in tumoroid re-stimulation assays, and in vivo anti-tumoral responses. Next, BEHAV3D video microscopy is used to assess CAR-T cell interaction with tumor cells at single cell resolution. These data are consistent with a threshold avidity of CAR-T / tumor cell interaction and target cell B7H3 expression level, where enhanced functionality is characterized by longer cumulative CD8⁺ CAR-T / tumor target interaction times, CAR-T cell expansion and sustained tumor control. Lower checkpoint receptor expression does not correlate with enhanced anti-tumor function. These results provide further insights into design of anti-B7H3 CAR-T cells for antigen-dim cell targeting, and avoidance of antigen-dim tumor relapse.

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抗b7h3 CAR-T构建体的功能亲和性预测触发效应功能的抗原密度阈值

嵌合抗原受体T细胞（CAR-T）治疗实体癌一直受到肿瘤微环境中与表达抗原的靶细胞相互作用后扩增和存活受限的影响。以B7H3作为具有广泛临床适用性的模型抗原，我们评估了三种临床候选结合物的抗体/抗原亲和力与以下三个特征之间的关系：细胞亲和力，类肿瘤再刺激试验中持续细胞毒性的持续时间，以及体内抗肿瘤反应。接下来，使用BEHAV3D视频显微镜在单细胞分辨率下评估CAR-T细胞与肿瘤细胞的相互作用。这些数据与CAR-T /肿瘤细胞相互作用的阈值和靶细胞B7H3表达水平一致，其中增强的功能的特征是CD8+ CAR-T /肿瘤靶相互作用时间更长，CAR-T细胞扩增和持续的肿瘤控制。较低的检查点受体表达与增强的抗肿瘤功能无关。这些结果为设计抗b7h3 CAR-T细胞靶向抗原暗淡细胞和避免抗原暗淡肿瘤复发提供了进一步的见解。

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来源期刊

Nature Communications Biological Science Disciplines-

CiteScore

24.90

自引率

2.40%

发文量

6928

审稿时长

3.7 months

期刊介绍： Nature Communications, an open-access journal, publishes high-quality research spanning all areas of the natural sciences. Papers featured in the journal showcase significant advances relevant to specialists in each respective field. With a 2-year impact factor of 16.6 (2022) and a median time of 8 days from submission to the first editorial decision, Nature Communications is committed to rapid dissemination of research findings. As a multidisciplinary journal, it welcomes contributions from biological, health, physical, chemical, Earth, social, mathematical, applied, and engineering sciences, aiming to highlight important breakthroughs within each domain.