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Combination drug delivery via multilamellar vesicles enables targeting of tumor cells and tumor vasculature

Published Time:2020-12-29Views:927

Combination drug delivery via multilamellar vesicles enables targeting of tumor cells and tumor vasculature

 

Published: 19 February 2018

Author: Yarong Liu, Yu J. Kim, Natnaree Siriwon, Jennifer A. Rohrs, Zhiqiang Yu, Pin Wanga    

Journal: Biotechnology & Bioengineering   

 

Abstract

 

Blood vessel development is critical for the continued growth and progression of solid tumors and, therefore, makes an attractive target for improving cancer therapy. Indeed, vasculartargeted therapies have been extensively explored but they have shown minimal efficacy as monotherapies. Combretastatin A4 (CA4) is a tubulinbinding vascular disrupting agent that selectively targets the established tumor endothelium, causing rapid vascular beak down. Despite its potent anticancer potential, the drug has doselimiting side effects, particularly in the form of cardiovascular toxicity. Furthermore, its poor aqueous solubility and the resulting limited bioavailability hinder its antitumor activity in the clinic. To improve the therapeutic efficacy of CA4, we investigated its application as a combination therapy with doxorubicin (Dox) in a tumor vasculature targeted delivery vehicle: peptidemodified crosslinked multilamellar liposomal vesicles (cMLVs). In vitro cell culture studies showed that a tumor vasculaturetargeting peptide, RIF7, could facilitate higher cellular uptake of drugloaded cMLVs, and consequently enhance the antitumor efficacy in both drug resistant B16 mouse melanoma and human MDAMB231 breast cancer cells. In vivo, upon intravenous injection, targeted cMLVs could efficiently deliver both Dox and CA4 to significantly slow tumor growth through the specific interaction of the targeting peptide with its receptor on the surface of tumor vasculature. This study demonstrates the potential of our novel targeted combination therapy delivery vehicle to improve the outcome of cancer treatment.    Go to Article Link


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