Issue 11, 2016

In situ crosslinked smart polypeptide nanoparticles for multistage responsive tumor-targeted drug delivery

Abstract

Smart tumor-targeted drug delivery is crucial for improving the effect of chemotherapy and reducing the adverse effects. Here, we synthesized a smart polypeptide copolymer based on n-butylamine-poly(L-lysine)-b-poly(L-cysteine) (PLL-PLC) with functionalization of folic acid (FA) and 1,2-dicarboxylic-cyclohexene anhydride (DCA) for multistage responsive tumor-targeted drug delivery. The copolymers (FA-PLL(DCA)-PLC) spontaneously crosslinked in situ to form redox and pH dual responsive FA-PLL(DCA)-PLC nanoparticles (FD-NPs), which had a reversible zeta potential around −30 mV at pH 7.4, but switched to +15 mV at pH 5.0. Moreover, FD-NPs effectively loaded DOX with a loading capacity at 15.7 wt%. At pH 7.4, only 24.5% DOX was released within 60 h. However, at pH 5.0, the presence of 10 mM DTT dramatically accelerated DOX release with over 90% of DOX released within 10 h. Although the FD-NPs only enhanced DOX uptake in FA receptor positive (FR+) cancer cells at pH 7.4, a weak acidic condition promoted FD-NP-facilitated DOX uptake in both FR+ HeLa and FR− A549 cells, as well as significantly improving cellular binding and end/lysosomal escape. In vivo studies in a HeLa cancer model demonstrated that the charge-reversible FD-NPs delivered DOX into tumors more effectively than charge-irreversible nanoparticles. Hence, these multistage responsive FD-NPs would serve as highly efficient drug vectors for targeted cancer chemotherapy.

Graphical abstract: In situ crosslinked smart polypeptide nanoparticles for multistage responsive tumor-targeted drug delivery

Supplementary files

Article information

Article type
Paper
Submitted
22 Oct 2015
Accepted
16 Feb 2016
First published
18 Feb 2016

Nanoscale, 2016,8, 5985-5995

In situ crosslinked smart polypeptide nanoparticles for multistage responsive tumor-targeted drug delivery

H. Yi, P. Liu, N. Sheng, P. Gong, Y. Ma and L. Cai, Nanoscale, 2016, 8, 5985 DOI: 10.1039/C5NR07348K

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