| Literature DB >> 32572197 |
Suping Li1,2, Yinlong Zhang1,2, Shih-Hsin Ho3, Bozhao Li1, Meifang Wang1, Xiongwei Deng1, Na Yang1, Guangna Liu1, Zefang Lu1,2, Junchao Xu1,2, Quanwei Shi1,2, Jing-Yan Han4, Lirong Zhang5, Yan Wu6,7, Yuliang Zhao8,9,10, Guangjun Nie11,12,13.
Abstract
Drugs that induce thrombosis in the tumour vasculature have not resulted in long-term tumour eradication owing to tumour regrowth from tissue in the surviving rim of the tumour, where tumour cells can derive nutrients from adjacent non-tumoral blood vessels and tissues. Here, we report the performance of a combination of tumour-infarction therapy and chemotherapy, delivered via chitosan-based nanoparticles decorated with a tumour-homing peptide targeting fibrin-fibronectin complexes overexpressed on tumour-vessel walls and in tumour stroma, and encapsulating the coagulation-inducing protease thrombin and the chemotherapeutic doxorubicin. Systemic administration of the nanoparticles into mice and rabbits bearing subcutaneous or orthotopic tumours resulted in higher tumour growth suppression and decreased tumour recurrence than nanoparticles delivering only thrombin or doxorubicin, with histological and haematological analyses indicating an absence of detectable toxicity. The co-administration of a cytotoxic payload and a protease to elicit vascular infarction in tumours with biodegradable tumour-targeted nanoparticles represents a promising strategy for improving the therapeutic index of coagulation-based tumour therapy.Entities:
Year: 2020 PMID: 32572197 DOI: 10.1038/s41551-020-0573-2
Source DB: PubMed Journal: Nat Biomed Eng ISSN: 2157-846X Impact factor: 25.671