Manganese Galvanic Cells Intervene in Tumor Metabolism to Reinforce cGAS-STING Activation for Bidirectional Synergistic Hydrogen-Immunotherapy

IF 26.8 1区 材料科学 Q1 CHEMISTRY, MULTIDISCIPLINARY Advanced Materials Pub Date : 2025-01-07 DOI:10.1002/adma.202414929
Nailin Yang, Shumin Sun, Jiachen Xu, Fei Gong, Huali Lei, Yu Hao, Zifan Pei, Chenya Wang, Qiao Yu, Jihu Nie, Nan Jiang, Caifang Ni, Liang Cheng
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Abstract

The cGAS-STING pathway is pivotal in initiating antitumor immunity. However, tumor metabolism, particularly glycolysis, negatively regulates the activation of the cGAS-STING pathway. Herein, Mn galvanic cells (MnG) are prepared via liquid-phase exfoliation and in situ galvanic replacement to modulate tumor metabolism, thereby enhancing cGAS-STING activation for bidirectional synergistic H2-immunotherapy. The obtained MnG can be etched by water, enabling efficient and sustained generation of H2 gas and Mn2+. MnG not only activated and amplified the cGAS-STING pathway through the sustained release of Mn2+ but also regulated tumor glucose metabolism to inhibit the expression of three prime repair exonuclease 2 (TREX2), thereby synergistically enhancing the activation of the cGAS-STING pathway. The injection of MnG into tumors resulted in a robust immune response, thereby providing favorable support for antitumor therapy. Consequently, the combination of MnG with immune checkpoint blockade therapy resulted in significant suppression of both primary tumors and distant tumors. Furthermore, the MnG-lipiodol dispersion exhibited remarkable efficacy in combination with transarterial embolization (TAE)-gas-immunotherapy in a rabbit orthotopic liver tumor model. The present study underscores the significance of employing a metal galvanic cell strategy for enhanced immunotherapy, thereby offering a novel approach for rational design of bioactive materials to augment immunotherapeutic effectiveness.

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锰原细胞干预肿瘤代谢增强cGAS-STING激活双向协同氢免疫治疗
cGAS-STING通路在启动抗肿瘤免疫中起关键作用。然而,肿瘤代谢,特别是糖酵解,负向调节cGAS-STING通路的激活。本研究通过液相剥脱和原位电替代制备Mn原细胞(Mn galvanic cells, MnG)来调节肿瘤代谢,从而增强cGAS-STING的激活,实现双向协同h2免疫治疗。所得的MnG可以被水蚀刻,从而有效和持续地生成H2气体和Mn2+。MnG不仅可以通过Mn2+的持续释放激活和扩增cGAS-STING通路,还可以通过调节肿瘤糖代谢抑制3 prime修复外切酶2 (TREX2)的表达,从而协同增强cGAS-STING通路的激活。将MnG注射到肿瘤中可产生强大的免疫反应,从而为抗肿瘤治疗提供有利的支持。因此,MnG联合免疫检查点阻断疗法对原发肿瘤和远处肿瘤均有显著的抑制作用。此外,在兔原位肝肿瘤模型中,mg -脂醇分散体联合经动脉栓塞(TAE)-气体免疫治疗显示出显著的疗效。本研究强调了采用金属原细胞策略增强免疫治疗的重要性,从而为合理设计生物活性材料以增强免疫治疗效果提供了一种新的方法。
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来源期刊
Advanced Materials
Advanced Materials 工程技术-材料科学:综合
CiteScore
43.00
自引率
4.10%
发文量
2182
审稿时长
2 months
期刊介绍: Advanced Materials, one of the world's most prestigious journals and the foundation of the Advanced portfolio, is the home of choice for best-in-class materials science for more than 30 years. Following this fast-growing and interdisciplinary field, we are considering and publishing the most important discoveries on any and all materials from materials scientists, chemists, physicists, engineers as well as health and life scientists and bringing you the latest results and trends in modern materials-related research every week.
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