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Camptothecin-based prodrug nanomedicines for cancer therapy

Renshuai Zhang, Jing Yu, Zhu Guo, Hongfei Jiang, Chao Wang

2023Nanoscale36 citationsDOI

Abstract

blocking DNA topoisomerase 1. Despite its encouraging and wide-spectrum antitumour activity, its application is significantly restricted owing to its instability, low solubility, significant toxicity, and acquired tumour cell resistance. This has resulted in the development of many CPT-based therapeutic agents, especially CPT-based nanomedicines, with improved pharmacokinetic and pharmacodynamic profiles. Specifically, smart CPT-based prodrug nanomedicines with stimuli-responsive release capacity have been extensively explored owing to the advantages such as high drug loading, improved stability, and decreased potential toxicity caused by the carrier materials in comparison with normal nanodrugs and traditional delivery systems. In this review, the potential strategies and applications of CPT-based nanoprodrugs for enhanced CPT delivery toward cancer cells are summarized. We appraise in detail the chemical structures and release mechanisms of these nanoprodrugs and guide materials chemists to develop more powerful nanomedicines that have real clinical therapeutic capacities.

Topics & Concepts

CamptothecinProdrugTopoisomeraseCancer therapyIrinotecanCytotoxic T cellCancer cellCancerPharmacologyDNAChemistryCancer researchMedicineBiochemistryIn vitroInternal medicineColorectal cancerNanoplatforms for cancer theranosticsCancer therapeutics and mechanismsAdvanced biosensing and bioanalysis techniques
Camptothecin-based prodrug nanomedicines for cancer therapy | Litcius