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Riboflavin photoactivation by upconversion nanoparticles for cancer treatment.


ABSTRACT: Riboflavin (Rf) is a vitamin and endogenous photosensitizer capable to generate reactive oxygen species (ROS) under UV-blue irradiation and kill cancer cells, which are characterized by the enhanced uptake of Rf. We confirmed its phototoxicity on human breast adenocarcinoma cells SK-BR-3 preincubated with 30-?M Rf and irradiated with ultraviolet light, and proved that such Rf concentrations (60??M) are attainable in vivo in tumour site by systemic intravascular injection. In order to extend the Rf photosensitization depth in cancer tissue to 6?mm in depth, we purpose-designed core/shell upconversion nanoparticles (UCNPs, NaYF4:Yb3+:Tm3+/NaYF4) capable to convert 2% of the deeply-penetrating excitation at 975?nm to ultraviolet-blue power. This power was expended to photosensitise Rf and kill SK-BR-3 cells preincubated with UCNPs and Rf, where the UCNP-Rf energy transfer was photon-mediated with ~14% Förster process contribution. SK-BR-3 xenograft regression in mice was observed for 50 days, following the Rf-UCNPs peritumoural injection and near-infrared light photodynamic treatment of the lesions.

SUBMITTER: Khaydukov EV 

PROVIDER: S-EPMC5059683 | biostudies-literature | 2016 Oct

REPOSITORIES: biostudies-literature

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Riboflavin photoactivation by upconversion nanoparticles for cancer treatment.

Khaydukov E V EV   Mironova K E KE   Semchishen V A VA   Generalova A N AN   Nechaev A V AV   Khochenkov D A DA   Stepanova E V EV   Lebedev O I OI   Zvyagin A V AV   Deyev S M SM   Panchenko V Ya VY  

Scientific reports 20161012


Riboflavin (Rf) is a vitamin and endogenous photosensitizer capable to generate reactive oxygen species (ROS) under UV-blue irradiation and kill cancer cells, which are characterized by the enhanced uptake of Rf. We confirmed its phototoxicity on human breast adenocarcinoma cells SK-BR-3 preincubated with 30-μM Rf and irradiated with ultraviolet light, and proved that such Rf concentrations (60 μM) are attainable in vivo in tumour site by systemic intravascular injection. In order to extend the  ...[more]

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