Homotypic biomimetic nanotheranostics enhance locoregional Cherenkov radiation-induced photodynamic therapy and ferroptosis in early bone metastases.
1/5 보강
Theranostics for deep-seated and multifocal bone metastases using conventional nanoparticulate strategies face significant challenges due to limited targeting and insufficient spatial controllability
APA
Xue R, Li S, et al. (2025). Homotypic biomimetic nanotheranostics enhance locoregional Cherenkov radiation-induced photodynamic therapy and ferroptosis in early bone metastases.. Journal of controlled release : official journal of the Controlled Release Society, 385, 113971. https://doi.org/10.1016/j.jconrel.2025.113971
MLA
Xue R, et al.. "Homotypic biomimetic nanotheranostics enhance locoregional Cherenkov radiation-induced photodynamic therapy and ferroptosis in early bone metastases.." Journal of controlled release : official journal of the Controlled Release Society, vol. 385, 2025, pp. 113971.
PMID
40545201 ↗
Abstract 한글 요약
Theranostics for deep-seated and multifocal bone metastases using conventional nanoparticulate strategies face significant challenges due to limited targeting and insufficient spatial controllability within the lesions. Here, we developed a sophisticated nanocarrier (MC@MH) camouflaged with the homologous prostate cancer cell membrane and ferritin-homing peptide (HKN). Following systemic injection, the biomimetic nanotheranostics preferentially accumulated in bone metastases through a homotypic targeting mechanism. The acidic/HO-rich microenvironment triggered the degradation of MnO in MC@MH, leading to the release of Mn ions that enhance magnetic resonance imaging (MRI) for bone metastases, particularly at early stages. The HKN further promoted interactions between MC@MH and intracellular ferritin. Guided by MRI, the separately administrated radionuclide (Ga-PSMA-617) also actively navigated to metastatic tumors. Based on the Cherenkov radiation effect, it served as a light source in the lesions, precisely irradiating the photosensitizer (Chlorin e6) released from MC@MH. The cytotoxic ROS generated from Cherenkov radiation-induced PDT not only destroyed cancer cells but also destructed ferritin to initiate a cascade of ferroptosis. Overall, our strategy facilitated bone remodeling and repair while preserving bone homeostasis, offering a novel avenue for locoregional and precise theranostics against metastatic cancer in vivo.
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