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Development of a Peptide-Based Nano-Sized Cathepsin B Inhibitor for Anticancer Therapy.


ABSTRACT: Numerous cathepsin B inhibitors have been developed and are under investigation as potential cancer treatments. They have been evaluated for their ability to inhibit cathepsin B activity and reduce tumor growth. However, they have shown critical limitations, including low anticancer efficacy and high toxicity, due to their low selectivity and delivery problems. In this study, we developed a novel peptide and drug conjugate (PDC)-based cathepsin B inhibitor using cathepsin-B-specific peptide (RR) and bile acid (BA). Interestingly, this RR and BA conjugate (RR-BA) was able to self-assemble in an aqueous solution, and as a result, it formed stable nanoparticles. The nano-sized RR-BA conjugate showed significant cathepsin B inhibitory effects and anticancer effects against mouse colorectal cancer (CT26) cells. Its therapeutic effect and low toxicity were also confirmed in CT26 tumor-bearing mice after intravenous injection. Therefore, based on these results, the RR-BA conjugate could be developed as an effective anticancer drug candidate for inhibiting cathepsin B in anticancer therapy.

SUBMITTER: Park SH 

PROVIDER: S-EPMC10141979 | biostudies-literature | 2023 Apr

REPOSITORIES: biostudies-literature

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Development of a Peptide-Based Nano-Sized Cathepsin B Inhibitor for Anticancer Therapy.

Park So-Hyeon SH   Lee Jun-Hyuck JH   Yang Seong-Bin SB   Lee Dong-Nyeong DN   Kang Tae-Bong TB   Park Jooho J  

Pharmaceutics 20230403 4


Numerous cathepsin B inhibitors have been developed and are under investigation as potential cancer treatments. They have been evaluated for their ability to inhibit cathepsin B activity and reduce tumor growth. However, they have shown critical limitations, including low anticancer efficacy and high toxicity, due to their low selectivity and delivery problems. In this study, we developed a novel peptide and drug conjugate (PDC)-based cathepsin B inhibitor using cathepsin-B-specific peptide (RR)  ...[more]

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