4.7 Article

A Unique Multifunctional Nanoenzyme Tailored for Triggering Tumor Microenvironment Activated NIR-II Photoacoustic Imaging and Chemodynamic/Photothermal Combined Therapy

期刊

ADVANCED HEALTHCARE MATERIALS
卷 11, 期 3, 页码 -

出版社

WILEY
DOI: 10.1002/adhm.202102073

关键词

chemodynamic; photothermal combined cancer therapy; multifunctional nanoenzymes; NIR-II photoacoustic imaging; oxygen vacancy nanocomposites; tumor microenvironments

资金

  1. National Natural Science Foundation of China [21775030, 21874030, IRT-16R15]
  2. BAGUI Scholar Program

向作者/读者索取更多资源

The Ox-POM@Cu nanocomposite demonstrates unique enzymatic functions in the tumor microenvironment, including multi-element catalytic activity and NIR-II photoacoustic imaging capabilities. By reacting with glutathione and hydrogen peroxide, it performs photothermal therapy and chemodynamic therapy functions, effectively diagnosing and treating malignant tumors.
The accurate diagnosis and targeted therapy of malignant tumors face significant challenges. To address these, an oxidized molybdenum polyoxometalate-copper nanocomposite (Ox-POM@Cu) is designed and synthesized here. The doping with Cu determines the formation of oxygen vacancies, which can increase the carrier concentration in Ox-POM@Cu, accelerate electron transfer, and enhance the redox activity, thus playing an efficient catalytic role. The nanocomposite presents unique enzymatic functions characterized by a multielement catalytic activity in the tumor microenvironment (TME). In addition, it can be employed as an NIR-II photoacoustic imaging (PAI) probe and cancer therapy agent. First, it participates in a redox reaction with glutathione (GSH) in tumor tissues, activates the PAI and photothermal therapy functions via NIR-II irradiation, and depletes the GSH supply in cancerous cells. Subsequently, it catalyzes a Fenton-like reaction with H2O2 in tumor tissues to form hydroxyl radicals, thereby performing a chemodynamic therapy function. The findings show that the developed nanoenzyme is very efficient in the diagnosis and treatment of malignant tumors. This work not only provides a new strategy for the design of TME-induced NIR-II PAI but also presents new insights into enhanced cancer therapy.

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