| Literature DB >> 33716549 |
Qingxin Mu1, Guanyou Lin1, Zachary R Stephen1, Steve Chung1, Hui Wang1, Victoria K Patton2, Rachel N Gebhart3, Miqin Zhang1.
Abstract
Systemic delivery of hydrophobic anti-cancer drugs with nanocarriers, particularly for drug-resistant and metastatic cancer, remain a challenge because of the difficulty to achieve high drug loading, while maintaining a small hydrodynamic size and colloid stability in blood to ensure delivery of an efficacious amount of drug to tumor cells. Here we introduce a new approach to address this challenge. In this approach, nanofibers of larger size with good drug loading capacity are first constructed by a self-assembly process, and upon intravascular injection and interacting with serum proteins in vivo, these nanofibers break down into ultra-fine nanoparticles of smaller size that inherit the drug loading property from their parent nanofibers. We demonstrate the efficacy of this approach with a clinically available anti-cancer drug: paclitaxel (PTX). In vitro, the PTX-loaded nanoparticles enter cancer cells and induce cellular apoptosis. In vivo, they demonstrate prolonged circulation in blood, induce no systemic toxicity, and show high potency in inhibiting tumor growth and metastasis in both mouse models of aggressive, drug-resistant breast cancer and melanoma. This study points to a new strategy toward improved anti-cancer drug delivery and therapy.Entities:
Keywords: cancer; chitosan; drug delivery; nanofibers; nanoparticles; paclitaxel
Year: 2020 PMID: 33716549 PMCID: PMC7944405 DOI: 10.1016/j.mattod.2020.03.005
Source DB: PubMed Journal: Mater Today (Kidlington) ISSN: 1369-7021 Impact factor: 31.041