Sustained drug release and cancer treatment by an
injectable and biodegradable cyanoacrylate-based local drug delivery system
Zhang, T (Zhang, Tao)[ 1 ] ; Tang, YJ (Tang, Yongjia)[ 1 ] ; Zhang, W (Zhang, Wei)[ 1 ] ; Liu, S (Liu, Shan)[ 2 ] ; Zhao, YM (Zhao, Yumei)[ 1 ] ; Wang, W (Wang, Wei)[ 3 ] ; Wang, J (Wang, Jian)[ 1 ] ; Xu, L (Xu, Liang)[ 1 ] ; Liu, KL (Liu, Keliang)[ 1 ]
JOURNAL OF
MATERIALS CHEMISTRY B, 2018, 6(8): 1216-1225
DOI: 10.1039/c7tb03066e
WOS:000427155200007
Abstract
Sustained
drug release at specific sites is clinically favorable for the treatment of
many diseases. The discovery of new polymeric materials suitable for prolonging
drug release, improving therapeutic efficiency, and decreasing systemic
toxicity is always of great interest in local sustained-release drug delivery
systems (LSRDDSs). In this study, a new cross-linked cyanoacrylate (CA)-based
LSRDDS is developed, in which the drug depot consists of a formulation of
methoxyethyl cyanoacrylate (MOE-CA) with the cross-linking agent CA-PEG-CA. The
MOE-CA endowed the CA polymer with good degradability. The drug-release profile
could be affected by the structure and composition ratio of the
MOE-CA/CA-PEG-CA monomer. The liquid CA monomer could dissolve the drug without
using other solvents, and could polymerize into a solid glue just in a few
seconds after injection. An optimal formulation loaded with 5-fluorouracil
(J-Fu-1.25) showed excellent anticancer activity both in vitro and in vivo,
with 50% survival of the mice and no significant systemic toxicity detected
during the experiment. The CA depot might affect the blood flow in microvessels
of tumors, thus contributing to the synergetic anticancer effect of
5-fluorouracil. We believe that this work provides a practical, biodegradable,
and biocompatible LSRDDS for chemotherapeutic drug delivery that can also be
applied universally with various drugs for certain therapeutic aims.
