Carrier-free Nano-prodrugs for Minimally Invasive Cancer Therapy

Abstract

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 it possesses 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 a various kinds of triggers.

Supplementary files

Article information

Article type
Paper
Submitted
23 Apr 2024
Accepted
17 Jul 2024
First published
26 Jul 2024

Nanoscale, 2024, Accepted Manuscript

Carrier-free Nano-prodrugs for Minimally Invasive Cancer Therapy

K. Tanita, Y. Koseki, S. Kumar, F. Taemaitree, A. Mizutani, H. Nakatsuji, R. Suzuki, A. T. N. Dao, F. Fujishima, H. Tada, T. Ishiga, K. Saijo, C. Ishioka and H. Kasai, Nanoscale, 2024, Accepted Manuscript , DOI: 10.1039/D4NR01763C

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