4.8 Article

Biodegradable Ferrous Sulfide-Based Nanocomposites for Tumor Theranostics through Specific Intratumoral Acidosis-Induced Metabolic Symbiosis Disruption

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AMER CHEMICAL SOC
DOI: 10.1021/jacs.2c07669

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资金

  1. National Natural Science Foundation of China
  2. Natural Science Foundation of Beijing Municipality
  3. National Key R&D Program of China
  4. China - German Collaboration Project
  5. [52027801]
  6. [51631001]
  7. [2191001]
  8. [2017YFA0206301]
  9. [M-0199]

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The study introduces a tumor therapy strategy that disrupts intratumoral metabolic symbiosis by inducing acidosis for tumor elimination, using carbonic anhydrase inhibitor-modified ferrous sulfide nanoparticles. The nanoparticles also have dual-mode imaging capabilities.
Abnormal metabolic symbiosis is a typical characteristic that differentiates the tumor regions from healthy tissues and meanwhile maintains tumor survival. It is of great potential to disrupt intratumoral metabolic symbiosis in tumor therapy. Herein, we report a specific tumor therapy strategy through inducing acidosis to disrupt intratumoral metabolic symbiosis for tumor elimination, which is based on carbonic anhydrase inhibitor (CAI)modified ferrous sulfide nanoparticles (FeS-PEG-CAI NPs). The FeS-PEG-CAI NPs show the acid-responsive degradation capacity to release functional components, including CAI, Fe2+, and H2S, while remaining quite stable under normal physiological conditions. The generated CAI and H2S gas can not only disrupt the intracellular metabolic symbiosis to induce acidosis but also provide suitable circumstances for Fe2+-mediated Fenton reaction, producing abundant toxic hydroxyl radicals. Meanwhile, these NPs also show the dual-mode imaging capacity with photoacoustic and magnetic resonance imaging, which can dynamically monitor tumor location in the process of synergistic chemodynamic/photothermal/gas therapy. Overall, the developed FeS-PEG-CAI NPs exert their role of disrupting intratumoral metabolic symbiosis and other synergistic effects, which further enrich tumor treatment strategies.

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