4.8 Article

Cancer Cytomembrane-Cloaked Prussian Blue Nanoparticles Enhance the Efficacy of Mild-Temperature Photothermal Therapy by Disrupting Mitochondrial Functions of Cancer Cells

Journal

ACS APPLIED MATERIALS & INTERFACES
Volume 13, Issue 31, Pages 37563-37577

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsami.1c11138

Keywords

Prussian blue nanoparticles; lonidamine; mild-temperature photothermal therapy; heat shock proteins; cancer cell membrane

Funding

  1. National Marine Economic Innovation and Development Project [16PYY007SF17]
  2. National Natural Science Foundation of China [31800794]
  3. Science Research Foundation of National Health and Family Planning Commission of PRC [WKJ2016-2-22]
  4. United Fujian Provincial Health and Education Project for Tacking the Key Research [WKJ2016-2-22]
  5. Program for Innovative Research Team in Science and Technology in Fujian Province University
  6. Natural Science Foundation of Fujian Province of China [2015J05169]
  7. Subsidized Project for Postgraduates' Innovative Fund in Scientific Research of Huaqiao University [17011081003]
  8. Open Project of Key Laboratory of Cancer and Neurodegenerative Disease Transformation in Fujian Province [FMUCN-201801]
  9. Instrument Analysis Center of Huaqiao University

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Researchers have developed a nanosystem for mild-temperature photothermal therapy by using modified nanoparticles, achieving efficient treatment of cancer cells by disrupting ATP production. This innovative approach shows significant potential for various biomedical applications.
Despite its success against cancer, photothermal therapy (PTT) (>50 degrees C) suffers from several limitations such as triggering inflammation and facilitating immune escape and metastasis and also damage to the surrounding normal cells. Mild-temperature PTT has been proposed to override these shortcomings. We developed a nanosystem using HepG2 cancer cell membrane-cloaked zinc glutamate-modified Prussian blue nanoparticles with triphenylphosphine-conjugated lonidamine (HmPGTL NPs). This innovative approach achieved an efficient mild-temperature PTT effect by downregulating the production of intracellular ATP. This disrupts a section of heat shock proteins that cushion cancer cells against heat. The physicochemical properties, anti-tumor efficacy, and mechanisms of HmPGTL NPs both in vitro and in vivo were investigated. Moreover, the nanoparticles cloaked with the HepG2 cell membrane substantially prolonged the circulation time in vivo. Overall, the designed nanocomposites enhance the efficacy of mild-temperature PTT by disrupting the production of ATP in cancer cells. Thus, we anticipate that the mild-temperature PTT nanosystem will certainly present its enormous potential in various biomedical applications.

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