Clickable bisreactive small gold nanoclusters for preparing multifunctionalized nanomaterials: application to photouncaging of an anticancer molecule

In this study, we successfully synthesized a small-sized gold nanocluster (2 nm) coated with homogeneous tripeptides bearing azido and amino groups that enable facile multifunctionalizations. Using sodium phenoxide to reduce tetrachloroauric( iii ) acid in the presence of the cysteine-containing tri...

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Veröffentlicht in:Chemical science (Cambridge) 2024-01, Vol.15 (4), p.142-148
Hauptverfasser: Watanabe, Kenji, Mao, Qiyue, Zhang, Zhouen, Hata, Machi, Kodera, Masahito, Kitagishi, Hiroaki, Niwa, Takashi, Hosoya, Takamitsu
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Sprache:eng
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Zusammenfassung:In this study, we successfully synthesized a small-sized gold nanocluster (2 nm) coated with homogeneous tripeptides bearing azido and amino groups that enable facile multifunctionalizations. Using sodium phenoxide to reduce tetrachloroauric( iii ) acid in the presence of the cysteine-containing tripeptide, we efficiently prepared the gold nanoclusters without damaging the azido group. We then utilized this clickable bisreactive nanocluster as a versatile platform for synthesizing multifunctionalized gold nanomaterials. The resulting nanoclusters were conjugated with an anticancer compound connected to an indolizine moiety for photoinduced uncaging, a photodynamic therapy agent acting as a photosensitizer for uncaging, and a cyclic RGD peptide. The cytotoxicity of the multifunctionalized gold nanoclusters was demonstrated through red light irradiation of human lung cancer-derived A549 cells treated with the synthesized nanomaterials. The significant cytotoxicity exhibited by the cells underscores the potential utility of this method in advanced cancer therapies. 2 nm sized gold nanoclusters with azido and amino groups were synthesized. The gold nanoclusters were conjugated with a caged anticancer compound and a photosensitizer for photouncaging, resulting in photoinduced toxicity in cancer cells.
ISSN:2041-6520
2041-6539
DOI:10.1039/d3sc04365g