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Self-Assembled Micelles Composed of Doxorubicin Conjugated Y-Shaped PEG-Poly(glutamic acid)(2) Copolymers via Hydrazone Linkers
In this work, micelles composed of doxorubicin-conjugated Y-shaped copolymers (YMs) linked via an acid-labile linker were constructed. Y-shaped copolymers of mPEG-b-poly(glutamate-hydrazone-doxorubicin)(2) and linear copolymers of mPEG-b-poly(glutamate-hydrazone-doxorubicin) were synthesized and cha...
Autores principales: | , , , , , , , , , |
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
MDPI
2014
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6271086/ https://www.ncbi.nlm.nih.gov/pubmed/25116804 http://dx.doi.org/10.3390/molecules190811915 |
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author | Sui, Bowen Xu, Hui Jin, Jian Gou, Jingxin Liu, Jingshuo Tang, Xing Zhang, Yu Xu, Jinghua Zhang, Hongfeng Jin, Xiangqun |
author_facet | Sui, Bowen Xu, Hui Jin, Jian Gou, Jingxin Liu, Jingshuo Tang, Xing Zhang, Yu Xu, Jinghua Zhang, Hongfeng Jin, Xiangqun |
author_sort | Sui, Bowen |
collection | PubMed |
description | In this work, micelles composed of doxorubicin-conjugated Y-shaped copolymers (YMs) linked via an acid-labile linker were constructed. Y-shaped copolymers of mPEG-b-poly(glutamate-hydrazone-doxorubicin)(2) and linear copolymers of mPEG-b-poly(glutamate-hydrazone-doxorubicin) were synthesized and characterized. Particle size, size distribution, morphology, drug loading content (DLC) and drug release of the micelles were determined. Alterations in size and DLC of the micelles could be achieved by varying the hydrophobic block lengths. Moreover, at fixed DLCs, YMs showed a smaller diameter than micelles composed of linear copolymers (LMs). Also, all prepared micelles showed sustained release behaviors under physiological conditions over 72 h. DOX loaded in YMs was released more completely, with 30% more drug released in acid. The anti-tumor efficacy of the micelles against HeLa cells was evaluated by MTT assays, and YMs exhibited stronger cytotoxic effects than LMs in a dose- and time-dependent manner. Cellular uptake studied by CLSM indicated that YMs and LMs were readily taken up by HeLa cells. According to the results of this study, doxorubicin-conjugated Y-shaped PEG-(polypeptide)(2) copolymers showed advantages over linear copolymers, like assembling into smaller nanoparticles, faster drug release in acid, which may correspond to higher cellular uptake and enhanced extracellular/intracellular drug release, indicating their potential in constructing nano-sized drug delivery systems. |
format | Online Article Text |
id | pubmed-6271086 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2014 |
publisher | MDPI |
record_format | MEDLINE/PubMed |
spelling | pubmed-62710862018-12-27 Self-Assembled Micelles Composed of Doxorubicin Conjugated Y-Shaped PEG-Poly(glutamic acid)(2) Copolymers via Hydrazone Linkers Sui, Bowen Xu, Hui Jin, Jian Gou, Jingxin Liu, Jingshuo Tang, Xing Zhang, Yu Xu, Jinghua Zhang, Hongfeng Jin, Xiangqun Molecules Article In this work, micelles composed of doxorubicin-conjugated Y-shaped copolymers (YMs) linked via an acid-labile linker were constructed. Y-shaped copolymers of mPEG-b-poly(glutamate-hydrazone-doxorubicin)(2) and linear copolymers of mPEG-b-poly(glutamate-hydrazone-doxorubicin) were synthesized and characterized. Particle size, size distribution, morphology, drug loading content (DLC) and drug release of the micelles were determined. Alterations in size and DLC of the micelles could be achieved by varying the hydrophobic block lengths. Moreover, at fixed DLCs, YMs showed a smaller diameter than micelles composed of linear copolymers (LMs). Also, all prepared micelles showed sustained release behaviors under physiological conditions over 72 h. DOX loaded in YMs was released more completely, with 30% more drug released in acid. The anti-tumor efficacy of the micelles against HeLa cells was evaluated by MTT assays, and YMs exhibited stronger cytotoxic effects than LMs in a dose- and time-dependent manner. Cellular uptake studied by CLSM indicated that YMs and LMs were readily taken up by HeLa cells. According to the results of this study, doxorubicin-conjugated Y-shaped PEG-(polypeptide)(2) copolymers showed advantages over linear copolymers, like assembling into smaller nanoparticles, faster drug release in acid, which may correspond to higher cellular uptake and enhanced extracellular/intracellular drug release, indicating their potential in constructing nano-sized drug delivery systems. MDPI 2014-08-11 /pmc/articles/PMC6271086/ /pubmed/25116804 http://dx.doi.org/10.3390/molecules190811915 Text en © 2014 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/3.0/). |
spellingShingle | Article Sui, Bowen Xu, Hui Jin, Jian Gou, Jingxin Liu, Jingshuo Tang, Xing Zhang, Yu Xu, Jinghua Zhang, Hongfeng Jin, Xiangqun Self-Assembled Micelles Composed of Doxorubicin Conjugated Y-Shaped PEG-Poly(glutamic acid)(2) Copolymers via Hydrazone Linkers |
title | Self-Assembled Micelles Composed of Doxorubicin Conjugated Y-Shaped PEG-Poly(glutamic acid)(2) Copolymers via Hydrazone Linkers |
title_full | Self-Assembled Micelles Composed of Doxorubicin Conjugated Y-Shaped PEG-Poly(glutamic acid)(2) Copolymers via Hydrazone Linkers |
title_fullStr | Self-Assembled Micelles Composed of Doxorubicin Conjugated Y-Shaped PEG-Poly(glutamic acid)(2) Copolymers via Hydrazone Linkers |
title_full_unstemmed | Self-Assembled Micelles Composed of Doxorubicin Conjugated Y-Shaped PEG-Poly(glutamic acid)(2) Copolymers via Hydrazone Linkers |
title_short | Self-Assembled Micelles Composed of Doxorubicin Conjugated Y-Shaped PEG-Poly(glutamic acid)(2) Copolymers via Hydrazone Linkers |
title_sort | self-assembled micelles composed of doxorubicin conjugated y-shaped peg-poly(glutamic acid)(2) copolymers via hydrazone linkers |
topic | Article |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6271086/ https://www.ncbi.nlm.nih.gov/pubmed/25116804 http://dx.doi.org/10.3390/molecules190811915 |
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