Carrier-free nano-prodrugs for minimally invasive cancer therapy

An anticancer nanodrug with few side effects that does not require the use of a nanocarrier, polyethylene glycol, or other additives has been developed. We have fabricated nano-prodrugs (NPDs) composed only of homodimeric prodrugs of the anticancer agent SN-38, which contains a disulfide bond. The p...

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Veröffentlicht in:Nanoscale 2024-08, Vol.16 (32), p.15256-15264
Hauptverfasser: Tanita, Keita, Koseki, Yoshitaka, Kumar, Sanjay, Taemaitree, Farsai, Mizutani, Asuka, Nakatsuji, Hirotaka, Suzuki, Ryuju, Dao, Anh Thi Ngoc, Fujishima, Fumiyoshi, Tada, Hiroshi, Ishida, Takanori, Saijo, Ken, Ishioka, Chikashi, Kasai, Hitoshi
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Sprache:eng
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Zusammenfassung:An anticancer nanodrug with few side effects that does not require the use of a nanocarrier, polyethylene glycol, or other additives has been developed. We have fabricated nano-prodrugs (NPDs) composed only of homodimeric prodrugs of the anticancer agent SN-38, which contains a disulfide bond. The prodrugs are stable against hydrolysis but selectively release SN-38 when the disulfide bond is cleaved by glutathione, which is present in high concentrations in cancer cells. The best-performing NPDs showed good dispersion stability in nanoparticle form, and animal experiments revealed that they possess much higher antitumor activity than irinotecan, a clinically applied prodrug of SN-38. This performance was achieved by improving tumor accumulation due to the size effect and targeted drug release mechanism. The present study provides an insight into the development of non-invasive NPDs with high pharmacological activity, and also offers new possibilities for designing prodrug molecules that can release drugs in response to various kinds of triggers. SNC4DC, a dimer of SN-38 derivatives, has been synthesized. SNC4DC nanoparticles called nano-prodrugs are internalized into the cell and dissociate, and the active SN-38 is released after reduction of the S-S bond in the presence of GSH occurs.
ISSN:2040-3364
2040-3372
2040-3372
DOI:10.1039/d4nr01763c