1550 nm excitation-responsive upconversion nanoparticles to establish dual-photodynamic therapy against pancreatic tumors

The second near-infrared biological window b (NIR-IIb, 1500-1700 nm) is recently considered as the promising region for deeper tissue penetration. Herein, a nanocarrier for 1550 nm light-responsive dual-photodynamic therapy (PDT) is developed to efficiently boost singlet oxygen ( 1 O 2 ) generation....

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Veröffentlicht in:Journal of materials chemistry. B, Materials for biology and medicine Materials for biology and medicine, 2021-01, Vol.9 (3), p.694-79
Hauptverfasser: Pham, Khang-Yen, Wang, Liu-Chun, Hsieh, Chia-Ching, Hsu, Ya-Ping, Chang, Li-Chan, Su, Wen-Pin, Chien, Yi-Hsin, Yeh, Chen-Sheng
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Sprache:eng
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Zusammenfassung:The second near-infrared biological window b (NIR-IIb, 1500-1700 nm) is recently considered as the promising region for deeper tissue penetration. Herein, a nanocarrier for 1550 nm light-responsive dual-photodynamic therapy (PDT) is developed to efficiently boost singlet oxygen ( 1 O 2 ) generation. The dual-photosensitizers (PSs), rose bengal (RB) and chlorin e6 (Ce6), are carried by the silica-coated core-shell LiYbF 4 :Er@LiGdF 4 upconversion nanoparticles (UCNPs), forming UCNP/RB,Ce6. Following 1550 nm laser irradiation, the upconversion emission of UCNP/RB,Ce6 in both green (∼550 nm) and red (∼670 nm) colors is fully utilized to activate RB and Ce6, respectively. The simultaneous triggering of dual-PS generates an abundant amount of 1 O 2 resulting in boosted PDT efficacy. This dual-PDT nanocarrier presents an enhanced anticancer effect under single dose treatment in comparison with the single-PS ones from in vitro and in vivo treatments. The marriage between the boosted dual-PDT and 1550 nm light excitation is anticipated to provide a new avenue for non-invasive therapy. The marriage between 1550 nm (NIR-IIb) light excitation and dual-photodynamic therapy for upconversion UCNP@SiO 2 /RB,Ce6-PEG nanoparticles to generate 1 O 2 showing a synergetic effect against pancreatic tumors in vitro and in vivo .
ISSN:2050-750X
2050-7518
DOI:10.1039/d0tb02655g