Improving regorafenib's organ target precision via nano-assembly to change its delivery mode abolishes chemoresistance and liver metastasis of colorectal cancer
Jia Liu, Daan Fu, Kang Wang, Ye Yuan, Yan Deng, Lin Shi, Mingyi Li, Cheng Zhou, Xiaohuan Lu, Qiying Lv, Guobin Wang, Lin Wang, Zheng Wang
Journal:JOURNAL OF COLLOID AND INTERFACE SCIENCE
IF:8.13
DOI:10.1016/j.jcis.2021.08.179
PMID:34500422
Published:2021-08-30
research field:肿瘤学分子生物学转化医学细胞信号传导癌症生物学
Abstract
Distant metastases and chemotherapy repellency are the key causes of colorectal cancer (CRC)-related mortality. Regorafenib, an oral multi-kinase inhibitor approved for treating advanced CRC with distant metastases and/or chemo-resistance, however only improves median overall survival by 1.4 months. Such limited therapeutic effect is likely due to the low bioavailability of orally administered hydrophobic regorafenib. A regorafenib nanodrug is fabricated by one-step self-assembly with a clinically often-used fluorescent agent (indocyanine green) for overcoming regorafenib’s limitations, towards improving regorafenib’s therapeutic efficacy in advanced CRC. This nanodrug (nanoRF) was characterized, and its antitumor effects were assessed in three preclinical CRC models. NanoRF converts regorafenib’s delivery approach from oral to intravenous with a significantly high encapsulation efficacy of regorafenib (96%) and a long-time colloidal stability. Nanodrug (nanoRF) markedly prolongs regorafenib’s blood circulation by halving clearance rate, and enhances regorafenib’s tumor accumulation. Across three preclinical CRC models (xenografted tumor, chemodrug-resistant xenografted tumor, and liver metastasis), nanoRF drastically enhances regorafenib’s tumor inhibiting efficacy by 0.5–4 folds and effectively extends survival by 0.5–5 folds. This regorafenib nanodrug is a simple, safe, and efficient therapeutic nanodrug for treating advanced CRC with a ready-to-be-clinically-translated potential.
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