Nano-mechanical Immunoengineering: Nanoparticle Elasticity Reprograms Tumor-Associated Macrophages via Piezo1

材料科学 生物物理学 内化 膜曲率 纳米技术 癌细胞 弹性(物理) 内吞作用 机械敏感通道 细胞生物学 复合材料 化学 细胞 小泡 癌症 生物 受体 生物化学 离子通道 遗传学
作者
Zichen Yang,Yuge Zhao,Xiaoyou Zhang,Li Huang,Kun Wang,Jiuyuan Sun,Nana Chen,Weimin Yin,Shiyu Chen,Hui Zhi,Liangyi Xue,Lulu An,Rongjie Li,Haiqing Dong,Jin‐Fu Xu,Yan Li,Yongyong Li
出处
期刊:ACS Nano [American Chemical Society]
卷期号:18 (32): 21221-21235 被引量:8
标识
DOI:10.1021/acsnano.4c04614
摘要

The mechanical properties of nanoparticles play a crucial role in regulating nanobiointeractions, influencing processes such as blood circulation, tumor accumulation/penetration, and internalization into cancer cells. Consequently, they have a significant impact on drug delivery and therapeutic efficacy. However, it remains unclear whether and how macrophages alter their biological function in response to nanoparticle elasticity. Here, we report on the nano-mechanical biological effects resulting from the interactions between elastic silica nanoparticles (SNs) and macrophages. The SNs with variational elasticity Young's moduli ranging from 81 to 837 MPa were synthesized, and it was demonstrated that M2 [tumor-associated macrophages (TAMs)] could be repolarized to M1 by the soft SNs. Additionally, our findings revealed that cell endocytosis, membrane tension, the curvature protein Baiap2, and the cytoskeleton were all influenced by the elasticity of SNs. Moreover, the mechanically sensitive protein Piezo1 on the cell membrane was activated, leading to calcium ion influx, activation of the NF-κB pathway, and the initiation of an inflammatory response. In vivo experiments demonstrated that the softest 81 MPa SNs enhanced tumor penetration and accumulation and repolarized TAMs in intratumoral hypoxic regions, ultimately resulting in a significant inhibition of tumor growth. Taken together, this study has established a cellular feedback mechanism in response to nanoparticle elasticity, which induces plasma membrane deformation and subsequent activation of mechanosensitive signals. This provides a distinctive "nano-mechanical immunoengineering" strategy for reprogramming TAMs to enhance cancer immunotherapy.
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