PAI-1-driven SFRP2high cancer-associated fibroblasts hijack the abscopal effect of radioimmunotherapy

IF 48.8 1区医学 Q1 CELL BIOLOGY

Cancer Cell Pub Date : 2025-03-13 DOI:10.1016/j.ccell.2025.02.024

Yan-Pei Zhang, Ze-Qin Guo, Xiao-Ting Cai, Zi-Xuan Rong, Yuan Fang, Jia-Qi Chen, Kui-Mao Zhuang, Min-Jie Ruan, Si-Cong Ma, Le-Yi Lin, Duan-Duan Han, Yang-Si Li, Yuan-Yuan Wang, Jian Wang, Chuan-Hui Cao, Xin-Ran Tang, Qian-Kun Xie, Yue Chen, Yan Lin, Jia-Le Tan, Zhong-Yi Dong

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引用次数: 0

Abstract

The abscopal effect of radioimmunotherapy, wherein tumor shrinkage occurs beyond the irradiated field, is therapeutically promising but clinically rare. The mechanisms underlying this effect remain elusive. Here, in vivo genome-wide CRISPR screening identifies SFRP2 as a potential stromal regulator of the abscopal effect. SFRP2 exhibits cancer-associated fibroblast (CAF)-specific expression and radioimmunotherapy-mediated upregulation in unirradiated tumors. Conditional Sfrp2 knockout in CAFs boosts the abscopal effect by rewiring the vascular-immune microenvironment to promote CD8⁺ T cell recruitment to unirradiated tumors. In vivo lineage tracing reveals that elevated SFRP2 correlates with radioimmunotherapy-driven pericyte lineage commitment. Serum proteomics reveals that irradiated-tumor-secreted PAI-1 triggers distant tumor pericyte cell-fate transition into SFRP2^high CAFs via the LRP1/p65 axis. Pharmacologically blocking SFRP2 or PAI-1 enhances the abscopal effect in humanized patient-derived xenograft models. Our findings collectively illustrate that PAI-1-induced SFRP2^high CAFs serve as critical stromal regulator to hijack the abscopal effect, providing promising targets for enhancing radioimmunotherapy effectiveness.

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pai -1驱动的sfrp2高癌相关成纤维细胞劫持放射免疫治疗的体外效应

放射免疫治疗的体外效应，即肿瘤缩小发生在放疗区之外，在治疗上是有希望的，但在临床上很少见。这种效应背后的机制仍然难以捉摸。在这里，体内全基因组CRISPR筛选鉴定出SFRP2是体外效应的潜在基质调节因子。在未照射的肿瘤中，SFRP2表现出癌症相关成纤维细胞（CAF）特异性表达和放射免疫治疗介导的上调。CAFs中条件性的strp2基因敲除通过重新连接血管免疫微环境来促进CD8+ T细胞募集到未照射的肿瘤，从而增强了体外效应。体内谱系追踪显示，升高的SFRP2与放射免疫治疗驱动的周细胞谱系承诺相关。血清蛋白质组学显示，照射后的肿瘤分泌的PAI-1通过LRP1/p65轴触发远处肿瘤周细胞向高sfrp2 cas的转变。药理学阻断SFRP2或PAI-1可增强人源异种移植模型的体外作用。我们的研究结果共同表明，pai -1诱导的sfrp2高caf是劫持体外效应的关键基质调节剂，为提高放射免疫治疗的有效性提供了有希望的靶点。

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

Cancer Cell 医学-肿瘤学

CiteScore

55.20

自引率

1.20%

发文量

179

审稿时长

4-8 weeks

期刊介绍： Cancer Cell is a journal that focuses on promoting major advances in cancer research and oncology. The primary criteria for considering manuscripts are as follows: Major advances: Manuscripts should provide significant advancements in answering important questions related to naturally occurring cancers. Translational research: The journal welcomes translational research, which involves the application of basic scientific findings to human health and clinical practice. Clinical investigations: Cancer Cell is interested in publishing clinical investigations that contribute to establishing new paradigms in the treatment, diagnosis, or prevention of cancers. Insights into cancer biology: The journal values clinical investigations that provide important insights into cancer biology beyond what has been revealed by preclinical studies. Mechanism-based proof-of-principle studies: Cancer Cell encourages the publication of mechanism-based proof-of-principle clinical studies, which demonstrate the feasibility of a specific therapeutic approach or diagnostic test.