In vivo photodynamic therapy using upconversion nanoparticles as remote-controlled nanotransducers
Author(s) -
Niagara Muhammad Idris,
Muthu Kumara Gnanasammandhan,
Jing Zhang,
Paul C. Ho,
Ratha Mahendran,
Yong Zhang
Publication year - 2012
Publication title -
nature medicine
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 19.536
H-Index - 547
eISSN - 1546-170X
pISSN - 1078-8956
DOI - 10.1038/nm.2933
Subject(s) - photodynamic therapy , photosensitizer , in vivo , photon upconversion , singlet oxygen , fluorescence , nanoparticle , chemistry , nanotechnology , cancer research , photochemistry , biophysics , materials science , optoelectronics , oxygen , medicine , optics , luminescence , biology , physics , microbiology and biotechnology , organic chemistry
Conventional photodynamic therapy (PDT) is limited by the penetration depth of visible light needed for its activation. Here we used mesoporous-silica-coated upconversion fluorescent nanoparticles (UCNs) as a nanotransducer to convert deeply penetrating near-infrared light to visible wavelengths and a carrier of photosensitizers. We also used the multicolor-emission capability of the UCNs at a single excitation wavelength for simultaneous activation of two photosensitizers for enhanced PDT. We showed a greater PDT efficacy with the dual-photosensitizer approach compared to approaches using a single photosensitizer, as determined by enhanced generation of singlet oxygen and reduced cell viability. In vivo studies also showed tumor growth inhibition in PDT-treated mice by direct injection of UCNs into melanoma tumors or intravenous injection of UCNs conjugated with a tumor-targeting agent into tumor-bearing mice. As the first demonstration, to the best of our knowledge, of the photosensitizer-loaded UCN as an in vivo-targeted PDT agent, this finding may serve as a platform for future noninvasive deep-cancer therapy.
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