AI Article Synopsis

  • A new drug delivery system using silybin-conjugated chitosan (CS-SB) was created to enhance the oral absorption of doxorubicin (DOX).
  • The system utilizes self-assembled micelles that are small in size (about 168 nm), have a significant drug loading capacity (8.59%), and low critical micelle concentration (1.3 × 10 g/mL).
  • CS-SB micelles demonstrated improved oral bioavailability of DOX (up to 193% compared to traditional forms) and showed potential for reduced cardiotoxicity and effective cellular uptake through endocytosis.

Article Abstract

A drug delivery system based on silybin-conjugated chitosan (CS-SB) polymeric micelles was developed to improve the oral absorption of doxorubicin (DOX). SB was grafted to CS via succinic acid, and CS-SB was identified by H NMR and FT-IR. The DOX-loaded micelles were prepared by self-assembly, and the characteristics of micelles, including a small particle size of 167.8 ± 2.3 nm, a high drug loading capacity of 8.59%, and a low critical micelle concentration of 1.3 × 10 g/mL, were demonstrated. The micelles showed oral bioavailability of up to 193% versus DOX·HCl. The cytotoxicity test showed the biosafety of CS-SB and the potential of reductive DOX-induced cardiotoxicity. The inhibition of P-gp efflux and CYP3A4 enzyme in CS-SB micelles was confirmed by cellular uptake and enzyme activity inhibition tests. The endocytosis process of micelles was revealed by an endocytosis inhibition test. The findings exhibited the potential of CS-SB micelles in drug delivery.

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http://dx.doi.org/10.1021/acs.biomac.4c00628DOI Listing

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Article Synopsis
  • A new drug delivery system using silybin-conjugated chitosan (CS-SB) was created to enhance the oral absorption of doxorubicin (DOX).
  • The system utilizes self-assembled micelles that are small in size (about 168 nm), have a significant drug loading capacity (8.59%), and low critical micelle concentration (1.3 × 10 g/mL).
  • CS-SB micelles demonstrated improved oral bioavailability of DOX (up to 193% compared to traditional forms) and showed potential for reduced cardiotoxicity and effective cellular uptake through endocytosis.
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