TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting

TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting

Feng-Ying Chen,1 Jing-Jing Yan,1 Han-Xi Yi,2 Fu-Qiang Hu,2 Yong-Zhong Du,2 Hong Yuan,2 Jian You,2 Meng-Dan Zhao1 1Women’s Hospital, School of Medicine, Zhejiang University, Hangzhou, People’s Republic of China; 2College of Pharmaceutical Science, Zhejiang University, Hangzhou,...

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Main Authors: Chen FY, Yan JJ, Yi HX, Hu FQ, Du YZ, Yuan H, You J, Zhao MD
Format: Article
Language:English
Published: Dove Medical Press 2014-09-01
Series:International Journal of Nanomedicine
Online Access:http://www.dovepress.com/tnyl-peptide-functional-chitosan-g-stearate-conjugate-micelles-for-tum-peer-reviewed-article-IJN
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spelling doaj-03183d1f0208473aab6b119a72579b282020-11-24T23:44:15ZengDove Medical PressInternational Journal of Nanomedicine1178-20132014-09-012014Issue 14597460818531TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targetingChen FYYan JJYi HXHu FQDu YZYuan HYou JZhao MD Feng-Ying Chen,1 Jing-Jing Yan,1 Han-Xi Yi,2 Fu-Qiang Hu,2 Yong-Zhong Du,2 Hong Yuan,2 Jian You,2 Meng-Dan Zhao1 1Women’s Hospital, School of Medicine, Zhejiang University, Hangzhou, People’s Republic of China; 2College of Pharmaceutical Science, Zhejiang University, Hangzhou, People’s Republic of China Abstract: Nowadays, a real challenge in cancer therapy is to design drug delivery systems that can achieve high concentrations of drugs at the target site for improved therapeutic effect with reduced side effects. In this research, we designed and synthesized a homing peptide-(TNYLFSPNGPIA, TNYL) modified chitosan-g-stearate (CS) polymer micelle (named T-CS) for targeting delivery. The peptide displayed specific binding affinity to EphB4 which is a member of the Eph family of receptor tyrosine protein kinases. The amphiphilic polymer T-CS can gather into micelles by themselves in an aqueous environment with a low critical micelle concentration value (91.2 µg/L) and nano-scaled size (82.1±2.8 nm). The drug encapsulation efficiency reached 86.43% after loading the hydrophobic drug doxorubicin (DOX). The cytotoxicity of T-CS/DOX against SKOV3 cells was enhanced by approximately 2.3-fold when compared with CS/DOX. The quantitative and qualitative analysis for cellular uptake indicated that TNYL modification can markedly increase cellular internalization in the EphB4-overexpressing SKOV3 cell line, especially with a short incubation time. It is interesting that relatively higher uptake of the T-CS/DOX micelles by SKOV3 cells (positive-EphB4) than A549 cells (negative-EphB4) was observed when the two cells were co-incubated. Furthermore, in vivo distribution experiment using a bilateral-tumor model showed that there was more fluorescence accumulation in the SKOV3 tumor than in the A549 tumor over the whole experiment. These results suggest that TNYL-modified CS micelles may be promising drug carriers as targeting therapy for the EphB4-overexpressing tumor. Keywords: chitosan-g-stearate, polymeric micelles, TNYL, active targeting, antitumor activityhttp://www.dovepress.com/tnyl-peptide-functional-chitosan-g-stearate-conjugate-micelles-for-tum-peer-reviewed-article-IJN
collection DOAJ
language English
format Article
sources DOAJ
author Chen FY
Yan JJ
Yi HX
Hu FQ
Du YZ
Yuan H
You J
Zhao MD
spellingShingle Chen FY
Yan JJ
Yi HX
Hu FQ
Du YZ
Yuan H
You J
Zhao MD
TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting
International Journal of Nanomedicine
author_facet Chen FY
Yan JJ
Yi HX
Hu FQ
Du YZ
Yuan H
You J
Zhao MD
author_sort Chen FY
title TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting
title_short TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting
title_full TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting
title_fullStr TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting
title_full_unstemmed TNYL peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting
title_sort tnyl peptide functional chitosan-g-stearate conjugate micelles for tumor specific targeting
publisher Dove Medical Press
series International Journal of Nanomedicine
issn 1178-2013
publishDate 2014-09-01
description Feng-Ying Chen,1 Jing-Jing Yan,1 Han-Xi Yi,2 Fu-Qiang Hu,2 Yong-Zhong Du,2 Hong Yuan,2 Jian You,2 Meng-Dan Zhao1 1Women’s Hospital, School of Medicine, Zhejiang University, Hangzhou, People’s Republic of China; 2College of Pharmaceutical Science, Zhejiang University, Hangzhou, People’s Republic of China Abstract: Nowadays, a real challenge in cancer therapy is to design drug delivery systems that can achieve high concentrations of drugs at the target site for improved therapeutic effect with reduced side effects. In this research, we designed and synthesized a homing peptide-(TNYLFSPNGPIA, TNYL) modified chitosan-g-stearate (CS) polymer micelle (named T-CS) for targeting delivery. The peptide displayed specific binding affinity to EphB4 which is a member of the Eph family of receptor tyrosine protein kinases. The amphiphilic polymer T-CS can gather into micelles by themselves in an aqueous environment with a low critical micelle concentration value (91.2 µg/L) and nano-scaled size (82.1±2.8 nm). The drug encapsulation efficiency reached 86.43% after loading the hydrophobic drug doxorubicin (DOX). The cytotoxicity of T-CS/DOX against SKOV3 cells was enhanced by approximately 2.3-fold when compared with CS/DOX. The quantitative and qualitative analysis for cellular uptake indicated that TNYL modification can markedly increase cellular internalization in the EphB4-overexpressing SKOV3 cell line, especially with a short incubation time. It is interesting that relatively higher uptake of the T-CS/DOX micelles by SKOV3 cells (positive-EphB4) than A549 cells (negative-EphB4) was observed when the two cells were co-incubated. Furthermore, in vivo distribution experiment using a bilateral-tumor model showed that there was more fluorescence accumulation in the SKOV3 tumor than in the A549 tumor over the whole experiment. These results suggest that TNYL-modified CS micelles may be promising drug carriers as targeting therapy for the EphB4-overexpressing tumor. Keywords: chitosan-g-stearate, polymeric micelles, TNYL, active targeting, antitumor activity
url http://www.dovepress.com/tnyl-peptide-functional-chitosan-g-stearate-conjugate-micelles-for-tum-peer-reviewed-article-IJN
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