Multichannel Sonocatalysis Amplifiers Target IDH1-Mutated Tumor Plasticity and Attenuate Ros Tolerance to Repress Malignant Cholangiocarcinoma
ADVANCED FUNCTIONAL MATERIALS(2023)
摘要
Tumor adaptation-originated tumor tolerance that compensatory mechanisms (e.g., isocitrate dehydrogenase (IDH) mutation) jointly shape is the dominant obstacle of ROS therapy. Currently, targeting a single pathway fails to fundamentally reverse the complex milieu and diminish tumor adaptation. Herein, a multichannel sonocatalysis amplifier is engineered via one-pot gas diffusion method to attenuate IDH1-mutated cholangiocarcinoma plasticity and tolerance to ROS therapy, wherein triptolide and IR780 are co-loaded in DSPE-mPEG-modified CaCO3 nanoparticles. Triptolide can blockade Nrf2 to cut off glutathione biosynthesis via blockading proteomic communication, and disrupt redox homeostasis to potentiate IR780-mediated sonocatalytic ROS production. ROS-induced mitochondria damages disrupt Ca2+ homeostasis and in turn aggravate ROS accumulation, which cooperates with sonocatalysis and Nrf2 blockade to reprogram mitochondrial energy and substance metabolism (e.g., adenosine triphosphatase and glutathione), hinder DNA self-repair, and impair IDH1-mutation-asired tolerance. Systematic experiments support that these actions in such multichannel sonocatalysis amplifiers indeed disrupt Ca2+/redox homeostasis to disarm robust tumor plasticity and IDH1-mutation-induced tolerance to sonocatalysis therapy against IDH1-mutated cholangiocarcinoma progression. Briefly, the sonocatalysis amplifiers pave a comprehensive avenue to reprogram tumor metabolism, target tumor vulnerability, and attenuate tumor plasticity against genomic instability-raised treatment adaptation.
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关键词
energetic and substantial metabolism reprogramming, IDH1-mutated cholangiocarcinoma, redox homeostasis, sonocatalysis amplifiers, tumor plasticity
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