Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben

Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben

Molecularly imprinted polymers (MIPs) are kinds of powerful materials with promising selective molecule recognition abilities. However, the conventional MIPs have relatively low binding capacity. In order to improve this characteristic of MIPs, the modification monomer based on β-cyclodextrin...

全面介紹

Saved in:
書目詳細資料
主要作者: Asman, Saliza
格式: Thesis
語言:English
出版: 2015
主題:
QD Chemistry
QD241-441 Organic chemistry
在線閱讀:http://eprints.uthm.edu.my/1745/1/24p%20SALIZA%20ASMAN.pdf
標簽: 添加標簽
沒有標簽, 成為第一個標記此記錄!
id my-uthm-ep.1745
record_format uketd_dc
spelling my-uthm-ep.17452021-10-10T04:40:16Z Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben 2015 Asman, Saliza QD Chemistry QD241-441 Organic chemistry Molecularly imprinted polymers (MIPs) are kinds of powerful materials with promising selective molecule recognition abilities. However, the conventional MIPs have relatively low binding capacity. In order to improve this characteristic of MIPs, the modification monomer based on β-cyclodextrin (β-CD) and the essential of reversible addition�fragmentation chain transfer (RAFT) polymerization process were studied to generate potential MIPs. The study focuses on the characterization and adsorption behaviour of MIPs for selective recognition of benzylparaben (BzP) analyte. The potential of β-CD in MIP was investigated by synthesizing a reversible addition-fragmentation chain transfer molecularly imprinted methacrylic acid functionalized β-cyclodextrin polymer; RAFT�MIP(MAA-β-CD) based on methacrylic acid functionalized β-cyclodextrin (MAA-β-CD) monomer, which was then compared to a reversible addition-fragmentation chain transfer molecularly imprinted methacrylic acid polymer; RAFT-MIP(MAA) synthesized without β-CD. Both MIPs were prepared by the RAFT polymerization process in bulk polymerization method. The resulting MIPs were characterized using Fourier Transform Infrared Spectroscopy (FTIR), Field Scanning Electron Microscope (FESEM) and Brunauer-Emmett-Teller (BET) analysis. The batch adsorption study that includes studying of the pH, kinetic, isotherm and thermodynamic was conducted. The essential of RAFT polymerization on MIP was studied by comparing RAFT-MIP(MAA-β-CD) with the molecularly imprinted methacrylic acid functionalized β-cyclodextrin polymer; MIP(MAA-β-CD) was synthesized without RAFT agent, and characterized by using FTIR, elemental analysis, FESEM and BET. The binding experiments demonstrated that the RAFT-MIP(MAA-β-CD) has a higher binding capacity and higher accessibility compared to RAFT-MIP(MAA) and MIP(MAA-β-CD) for selective of BzP, respectively. The β-CD and RAFT polymerization process improved the MIP’s physical properties and iv enhanced its recognition capacity, thus affecting the adsorption behaviour of RAFT�MIP(MAA-β-CD). The effects of RAFT polymerization process were also investigated by a reversible addition-fragmentation transfer molecularly imprinted hydroxylethyl methacrylate functionalized β-cyclodextrin polymer; RAFT-MIP(HEMA-β-CD). The RAFT-MIP(HEMA-β-CD) was synthesized based on the hydroxylethyl-methacrylate functionalized β-cyclodextrin (HEMA-β-CD) monomer and was prepared by the RAFT polymerization process in bulk polymerization method. The molecularly imprinted hydroxylethyl-methacrylate functionalized β-cyclodextrin polymer; MIP(HEMA-β-CD) without a RAFT agent was synthesized as comparison. A similar study to RAFT�MIP(MAA-β-CD) had also been carried out for RAFT-MIP(HEMA-β-CD).The effects of RAFT polymerization on RAFT-MIP(HEMA-β-CD) were contrasted with RAFT�MIP(MAA-β-CD). The compact and non-porous morphology of RAFT-MIP(HEMA-β�CD) reduces its binding capacity performance compared to MIP(HEMA-β-CD). Thus, this directly affected the RAFT-MIP(HEMA-β-CD) adsorption behaviour towards BzP. It was resulted that the RAFT polymerization had not improved the synthesis of RAFT�MIP(HEMA-β-CD). Careful choice of RAFT agent and monomer is essential in realizing good control over the RAFT-MIP polymerization process, and generating potential MIP. 2015 Thesis http://eprints.uthm.edu.my/1745/ http://eprints.uthm.edu.my/1745/1/24p%20SALIZA%20ASMAN.pdf text en public phd doctoral Universiti Malaya Fakulti Sains
institution Universiti Tun Hussein Onn Malaysia
collection UTHM Institutional Repository
language English
topic QD Chemistry
QD241-441 Organic chemistry
spellingShingle QD Chemistry
QD241-441 Organic chemistry
Asman, Saliza
Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben
description Molecularly imprinted polymers (MIPs) are kinds of powerful materials with promising selective molecule recognition abilities. However, the conventional MIPs have relatively low binding capacity. In order to improve this characteristic of MIPs, the modification monomer based on β-cyclodextrin (β-CD) and the essential of reversible addition�fragmentation chain transfer (RAFT) polymerization process were studied to generate potential MIPs. The study focuses on the characterization and adsorption behaviour of MIPs for selective recognition of benzylparaben (BzP) analyte. The potential of β-CD in MIP was investigated by synthesizing a reversible addition-fragmentation chain transfer molecularly imprinted methacrylic acid functionalized β-cyclodextrin polymer; RAFT�MIP(MAA-β-CD) based on methacrylic acid functionalized β-cyclodextrin (MAA-β-CD) monomer, which was then compared to a reversible addition-fragmentation chain transfer molecularly imprinted methacrylic acid polymer; RAFT-MIP(MAA) synthesized without β-CD. Both MIPs were prepared by the RAFT polymerization process in bulk polymerization method. The resulting MIPs were characterized using Fourier Transform Infrared Spectroscopy (FTIR), Field Scanning Electron Microscope (FESEM) and Brunauer-Emmett-Teller (BET) analysis. The batch adsorption study that includes studying of the pH, kinetic, isotherm and thermodynamic was conducted. The essential of RAFT polymerization on MIP was studied by comparing RAFT-MIP(MAA-β-CD) with the molecularly imprinted methacrylic acid functionalized β-cyclodextrin polymer; MIP(MAA-β-CD) was synthesized without RAFT agent, and characterized by using FTIR, elemental analysis, FESEM and BET. The binding experiments demonstrated that the RAFT-MIP(MAA-β-CD) has a higher binding capacity and higher accessibility compared to RAFT-MIP(MAA) and MIP(MAA-β-CD) for selective of BzP, respectively. The β-CD and RAFT polymerization process improved the MIP’s physical properties and iv enhanced its recognition capacity, thus affecting the adsorption behaviour of RAFT�MIP(MAA-β-CD). The effects of RAFT polymerization process were also investigated by a reversible addition-fragmentation transfer molecularly imprinted hydroxylethyl methacrylate functionalized β-cyclodextrin polymer; RAFT-MIP(HEMA-β-CD). The RAFT-MIP(HEMA-β-CD) was synthesized based on the hydroxylethyl-methacrylate functionalized β-cyclodextrin (HEMA-β-CD) monomer and was prepared by the RAFT polymerization process in bulk polymerization method. The molecularly imprinted hydroxylethyl-methacrylate functionalized β-cyclodextrin polymer; MIP(HEMA-β-CD) without a RAFT agent was synthesized as comparison. A similar study to RAFT�MIP(MAA-β-CD) had also been carried out for RAFT-MIP(HEMA-β-CD).The effects of RAFT polymerization on RAFT-MIP(HEMA-β-CD) were contrasted with RAFT�MIP(MAA-β-CD). The compact and non-porous morphology of RAFT-MIP(HEMA-β�CD) reduces its binding capacity performance compared to MIP(HEMA-β-CD). Thus, this directly affected the RAFT-MIP(HEMA-β-CD) adsorption behaviour towards BzP. It was resulted that the RAFT polymerization had not improved the synthesis of RAFT�MIP(HEMA-β-CD). Careful choice of RAFT agent and monomer is essential in realizing good control over the RAFT-MIP polymerization process, and generating potential MIP.
format Thesis
qualification_name Doctor of Philosophy (PhD.)
qualification_level Doctorate
author Asman, Saliza
author_facet Asman, Saliza
author_sort Asman, Saliza
title Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben
title_short Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben
title_full Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben
title_fullStr Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben
title_full_unstemmed Adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (RAFT) polymerization for selective recognition of benzylparaben
title_sort adsorption behaviour of molecularly imprinted-beta-cyclodextrin polymers prepared by reversible addition-fragmentation chain transfer (raft) polymerization for selective recognition of benzylparaben
granting_institution Universiti Malaya
granting_department Fakulti Sains
publishDate 2015
url http://eprints.uthm.edu.my/1745/1/24p%20SALIZA%20ASMAN.pdf
_version_ 1747830861094453248

相似書籍