Antibacterial modification of an injectable, biodegradable, non-cytotoxic block copolymer-based physical gel with body temperature-stimulated sol-gel transition and controlled drug release

Xiaowen Wang; Huawen Hu; Wenyi Wang; Ka I. Lee; Chang Gao; Liang He; Yuanfeng Wang; Chuilin Lai; Bin Fei; John H. Xin

doi:10.1016/j.colsurfb.2016.02.008

Antibacterial modification of an injectable, biodegradable, non-cytotoxic block copolymer-based physical gel with body temperature-stimulated sol-gel transition and controlled drug release

Xiaowen Wang, Huawen Hu, Wenyi Wang, Ka I. Lee, Chang Gao, Liang He, Yuanfeng Wang, Chuilin Lai, Bin Fei, John H. Xin

Research output: Journal article publication › Journal article › Academic research › peer-review

18 Citations (Scopus)

Abstract

Biomaterials are being extensively used in various biomedical fields; however, they are readily infected with microorganisms, thus posing a serious threat to the public health care. We herein presented a facile route to the antibacterial modification of an important A-B-A type biomaterial using poly (ethylene glycol) methyl ether (mPEG)- poly(ε-caprolactone) (PCL)-mPEG as a typical model. Inexpensive, commercial bis(2-hydroxyethyl) methylammonium chloride (DMA) was adopted as an antibacterial unit. The effective synthesis of the antibacterial copolymer mPEG-PCL-~~~-PCL-mPEG (where ~~~ denotes the segment with DMA units) was well confirmed by FTIR and ¹H NMR spectra. At an appropriate modification extent, the DMA unit could render the copolymer mPEG-PCL-~~~-PCL-mPEG highly antibacterial, but did not largely alter its fascinating intrinsic properties including the thermosensitivity (e.g., the body temperature-induced sol-gel transition), non-cytotoxicity, and controlled drug release. A detailed study on the sol-gel-sol transition behavior of different copolymers showed that an appropriate extent of modification with DMA retained a sol-gel-sol transition, despite the fact that a too high extent caused a loss of sol-gel-sol transition. The hydrophilic and hydrophobic balance between mPEG and PCL was most likely broken upon a high extent of quaternization due to a large disturbance effect of DMA units at a large quantity (as evidenced by the heavily depressed PCL segment crystallinity), and thus the micelle aggregation mechanism for the gel formation could not work anymore, along with the loss of the thermosensitivity. The work presented here is highly expected to be generalized for synthesis of various block copolymers with immunity to microorganisms. Light may also be shed on understanding the phase transition behavior of various multiblock copolymers.

Original language	English
Pages (from-to)	342-351
Number of pages	10
Journal	Colloids and Surfaces B: Biointerfaces
Volume	143
DOIs	https://doi.org/10.1016/j.colsurfb.2016.02.008
Publication status	Published - 1 Jul 2016

Keywords

Amphiphilic balance
Antibacterial modification
Crystallinity
MPEG-PCL-DMA-PCL-mPEG block copolymers
Sol-gel-sol transition

ASJC Scopus subject areas

Biotechnology
Surfaces and Interfaces
Physical and Theoretical Chemistry
Colloid and Surface Chemistry

More information

10.1016/j.colsurfb.2016.02.008

Cite this

Wang, X., Hu, H., Wang, W., Lee, K. I., Gao, C., He, L., Wang, Y., Lai, C., Fei, B., & Xin, J. H. (2016). Antibacterial modification of an injectable, biodegradable, non-cytotoxic block copolymer-based physical gel with body temperature-stimulated sol-gel transition and controlled drug release. Colloids and Surfaces B: Biointerfaces, 143, 342-351. https://doi.org/10.1016/j.colsurfb.2016.02.008

@article{ebd26875c9f8417181f6c6becb457054,

title = "Antibacterial modification of an injectable, biodegradable, non-cytotoxic block copolymer-based physical gel with body temperature-stimulated sol-gel transition and controlled drug release",

abstract = "Biomaterials are being extensively used in various biomedical fields; however, they are readily infected with microorganisms, thus posing a serious threat to the public health care. We herein presented a facile route to the antibacterial modification of an important A-B-A type biomaterial using poly (ethylene glycol) methyl ether (mPEG)- poly(ε-caprolactone) (PCL)-mPEG as a typical model. Inexpensive, commercial bis(2-hydroxyethyl) methylammonium chloride (DMA) was adopted as an antibacterial unit. The effective synthesis of the antibacterial copolymer mPEG-PCL-~~~-PCL-mPEG (where ~~~ denotes the segment with DMA units) was well confirmed by FTIR and 1H NMR spectra. At an appropriate modification extent, the DMA unit could render the copolymer mPEG-PCL-~~~-PCL-mPEG highly antibacterial, but did not largely alter its fascinating intrinsic properties including the thermosensitivity (e.g., the body temperature-induced sol-gel transition), non-cytotoxicity, and controlled drug release. A detailed study on the sol-gel-sol transition behavior of different copolymers showed that an appropriate extent of modification with DMA retained a sol-gel-sol transition, despite the fact that a too high extent caused a loss of sol-gel-sol transition. The hydrophilic and hydrophobic balance between mPEG and PCL was most likely broken upon a high extent of quaternization due to a large disturbance effect of DMA units at a large quantity (as evidenced by the heavily depressed PCL segment crystallinity), and thus the micelle aggregation mechanism for the gel formation could not work anymore, along with the loss of the thermosensitivity. The work presented here is highly expected to be generalized for synthesis of various block copolymers with immunity to microorganisms. Light may also be shed on understanding the phase transition behavior of various multiblock copolymers.",

keywords = "Amphiphilic balance, Antibacterial modification, Crystallinity, MPEG-PCL-DMA-PCL-mPEG block copolymers, Sol-gel-sol transition",

author = "Xiaowen Wang and Huawen Hu and Wenyi Wang and Lee, {Ka I.} and Chang Gao and Liang He and Yuanfeng Wang and Chuilin Lai and Bin Fei and Xin, {John H.}",

note = "Funding Information: We greatly appreciate the PolyU 5316/10E funding from Research Grants Council of the Hong Kong SAR Government . Publisher Copyright: {\textcopyright} 2016 Elsevier B.V.",

year = "2016",

month = jul,

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doi = "10.1016/j.colsurfb.2016.02.008",

language = "English",

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Wang, X, Hu, H, Wang, W, Lee, KI, Gao, C, He, L, Wang, Y, Lai, C, Fei, B & Xin, JH 2016, 'Antibacterial modification of an injectable, biodegradable, non-cytotoxic block copolymer-based physical gel with body temperature-stimulated sol-gel transition and controlled drug release', Colloids and Surfaces B: Biointerfaces, vol. 143, pp. 342-351. https://doi.org/10.1016/j.colsurfb.2016.02.008

Antibacterial modification of an injectable, biodegradable, non-cytotoxic block copolymer-based physical gel with body temperature-stimulated sol-gel transition and controlled drug release. / Wang, Xiaowen; Hu, Huawen; Wang, Wenyi et al.
In: Colloids and Surfaces B: Biointerfaces, Vol. 143, 01.07.2016, p. 342-351.

Research output: Journal article publication › Journal article › Academic research › peer-review

TY - JOUR

T1 - Antibacterial modification of an injectable, biodegradable, non-cytotoxic block copolymer-based physical gel with body temperature-stimulated sol-gel transition and controlled drug release

AU - Wang, Xiaowen

AU - Hu, Huawen

AU - Wang, Wenyi

AU - Lee, Ka I.

AU - Gao, Chang

AU - He, Liang

AU - Wang, Yuanfeng

AU - Lai, Chuilin

AU - Fei, Bin

AU - Xin, John H.

PY - 2016/7/1

Y1 - 2016/7/1

N2 - Biomaterials are being extensively used in various biomedical fields; however, they are readily infected with microorganisms, thus posing a serious threat to the public health care. We herein presented a facile route to the antibacterial modification of an important A-B-A type biomaterial using poly (ethylene glycol) methyl ether (mPEG)- poly(ε-caprolactone) (PCL)-mPEG as a typical model. Inexpensive, commercial bis(2-hydroxyethyl) methylammonium chloride (DMA) was adopted as an antibacterial unit. The effective synthesis of the antibacterial copolymer mPEG-PCL-~~~-PCL-mPEG (where ~~~ denotes the segment with DMA units) was well confirmed by FTIR and 1H NMR spectra. At an appropriate modification extent, the DMA unit could render the copolymer mPEG-PCL-~~~-PCL-mPEG highly antibacterial, but did not largely alter its fascinating intrinsic properties including the thermosensitivity (e.g., the body temperature-induced sol-gel transition), non-cytotoxicity, and controlled drug release. A detailed study on the sol-gel-sol transition behavior of different copolymers showed that an appropriate extent of modification with DMA retained a sol-gel-sol transition, despite the fact that a too high extent caused a loss of sol-gel-sol transition. The hydrophilic and hydrophobic balance between mPEG and PCL was most likely broken upon a high extent of quaternization due to a large disturbance effect of DMA units at a large quantity (as evidenced by the heavily depressed PCL segment crystallinity), and thus the micelle aggregation mechanism for the gel formation could not work anymore, along with the loss of the thermosensitivity. The work presented here is highly expected to be generalized for synthesis of various block copolymers with immunity to microorganisms. Light may also be shed on understanding the phase transition behavior of various multiblock copolymers.

AB - Biomaterials are being extensively used in various biomedical fields; however, they are readily infected with microorganisms, thus posing a serious threat to the public health care. We herein presented a facile route to the antibacterial modification of an important A-B-A type biomaterial using poly (ethylene glycol) methyl ether (mPEG)- poly(ε-caprolactone) (PCL)-mPEG as a typical model. Inexpensive, commercial bis(2-hydroxyethyl) methylammonium chloride (DMA) was adopted as an antibacterial unit. The effective synthesis of the antibacterial copolymer mPEG-PCL-~~~-PCL-mPEG (where ~~~ denotes the segment with DMA units) was well confirmed by FTIR and 1H NMR spectra. At an appropriate modification extent, the DMA unit could render the copolymer mPEG-PCL-~~~-PCL-mPEG highly antibacterial, but did not largely alter its fascinating intrinsic properties including the thermosensitivity (e.g., the body temperature-induced sol-gel transition), non-cytotoxicity, and controlled drug release. A detailed study on the sol-gel-sol transition behavior of different copolymers showed that an appropriate extent of modification with DMA retained a sol-gel-sol transition, despite the fact that a too high extent caused a loss of sol-gel-sol transition. The hydrophilic and hydrophobic balance between mPEG and PCL was most likely broken upon a high extent of quaternization due to a large disturbance effect of DMA units at a large quantity (as evidenced by the heavily depressed PCL segment crystallinity), and thus the micelle aggregation mechanism for the gel formation could not work anymore, along with the loss of the thermosensitivity. The work presented here is highly expected to be generalized for synthesis of various block copolymers with immunity to microorganisms. Light may also be shed on understanding the phase transition behavior of various multiblock copolymers.

KW - Amphiphilic balance

KW - Antibacterial modification

KW - Crystallinity

KW - MPEG-PCL-DMA-PCL-mPEG block copolymers

KW - Sol-gel-sol transition

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DO - 10.1016/j.colsurfb.2016.02.008

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AN - SCOPUS:84962321917

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Antibacterial modification of an injectable, biodegradable, non-cytotoxic block copolymer-based physical gel with body temperature-stimulated sol-gel transition and controlled drug release

Abstract

Keywords

ASJC Scopus subject areas

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