Development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies
In the first part of this work, magnetized nanoporous silica based microparticles (MMPs) are used for horseradish peroxidase (HRP) immobilization and applied in amperometric peroxidase-based biosensors. A homemade magnetized carbon paste electrode permits the MMPs attraction close to the electrode s...
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Universite Libre de Bruxelles
2008
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Online Access: | http://theses.ulb.ac.be/ETD-db/collection/available/ULBetd-06092008-110943/ |
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Magnetic particles Capillary electrophoresis Biosensors Microreactors |
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Magnetic particles Capillary electrophoresis Biosensors Microreactors Yu, Donghui Development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies |
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In the first part of this work, magnetized nanoporous silica based microparticles (MMPs) are used for horseradish peroxidase (HRP) immobilization and applied in amperometric peroxidase-based biosensors. A homemade magnetized carbon paste electrode permits the MMPs attraction close to the electrode surface. The resulting original biosensor is applied to the investigation of enzymatic oxidation of model drug compounds namely, clozapine (CLZ) and acetaminophen (APAP) by HRP in the presence of hydrogen peroxide. The biosensor operates at a low applied potential and the signal corresponds to the electro-reduction of electroactive species enzymatically generated. The biosensor allows performing the quantitation of the two drug compounds in the micromolar concentration range. It allows also the study of thiol compounds based on the inhibition of the biosensor response. Interestingly, distinct inhibition results are observed for HRP entrapped in the silica microparticles compared to the soluble HRP.
We expect that this type of biosensors holds high promise in quantitative analysis and in biotransformation studies of drug compounds.
In the second part of this thesis work, HRP immobilized magnetic nanoparticles are injected on-line and magnetically retained, as a microreactor, in the capillary of a CE setup. The purpose of such a configuration is to develop an analytical tool for studying “in vitro” drug biotransformation. The advantages expected are (i) minimum sample (drug compound) and biocomponent (enzyme) consumption, (ii) high analysis throughput, (iii) selectivity and sensitivity. In order to illustrate the potential of such an instrumental configuration, it has been applied to study acetaminophen as model drug compound. The mechanistic information obtained by the HRP/H2O2 system is in agreement with literature data on acetaminophen metabolization. Horseradish peroxidase kinetic studies are realized by this setup and the apparent Michaelis constant is determined. Capillary electrophoresis permitted the identification of APAP off-line biotransformed products such as N-acetyl-p-benzoquinone imine (NAPQI), the APAP dimer and APAP polymers as inferred from literature data. The formation of the APAP dimer was further confirmed by electrospray ionization mass spectrometry.
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author2 |
Van Schepdael Ann |
author_facet |
Van Schepdael Ann Yu, Donghui |
author |
Yu, Donghui |
author_sort |
Yu, Donghui |
title |
Development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies |
title_short |
Development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies |
title_full |
Development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies |
title_fullStr |
Development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies |
title_full_unstemmed |
Development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies |
title_sort |
development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies |
publisher |
Universite Libre de Bruxelles |
publishDate |
2008 |
url |
http://theses.ulb.ac.be/ETD-db/collection/available/ULBetd-06092008-110943/ |
work_keys_str_mv |
AT yudonghui developmentofmagneticparticlebasedbiosensorsandmicroreactorsfordruganalysisandbiotransformationstudies |
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1716393969331470336 |
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ndltd-BICfB-oai-ulb.ac.be-ETDULB-ULBetd-06092008-1109432013-01-07T15:43:29Z Development of magnetic particle based biosensors and microreactors for drug analysis and biotransformation studies Yu, Donghui Magnetic particles Capillary electrophoresis Biosensors Microreactors In the first part of this work, magnetized nanoporous silica based microparticles (MMPs) are used for horseradish peroxidase (HRP) immobilization and applied in amperometric peroxidase-based biosensors. A homemade magnetized carbon paste electrode permits the MMPs attraction close to the electrode surface. The resulting original biosensor is applied to the investigation of enzymatic oxidation of model drug compounds namely, clozapine (CLZ) and acetaminophen (APAP) by HRP in the presence of hydrogen peroxide. The biosensor operates at a low applied potential and the signal corresponds to the electro-reduction of electroactive species enzymatically generated. The biosensor allows performing the quantitation of the two drug compounds in the micromolar concentration range. It allows also the study of thiol compounds based on the inhibition of the biosensor response. Interestingly, distinct inhibition results are observed for HRP entrapped in the silica microparticles compared to the soluble HRP. We expect that this type of biosensors holds high promise in quantitative analysis and in biotransformation studies of drug compounds. In the second part of this thesis work, HRP immobilized magnetic nanoparticles are injected on-line and magnetically retained, as a microreactor, in the capillary of a CE setup. The purpose of such a configuration is to develop an analytical tool for studying “in vitro” drug biotransformation. The advantages expected are (i) minimum sample (drug compound) and biocomponent (enzyme) consumption, (ii) high analysis throughput, (iii) selectivity and sensitivity. In order to illustrate the potential of such an instrumental configuration, it has been applied to study acetaminophen as model drug compound. The mechanistic information obtained by the HRP/H2O2 system is in agreement with literature data on acetaminophen metabolization. Horseradish peroxidase kinetic studies are realized by this setup and the apparent Michaelis constant is determined. Capillary electrophoresis permitted the identification of APAP off-line biotransformed products such as N-acetyl-p-benzoquinone imine (NAPQI), the APAP dimer and APAP polymers as inferred from literature data. The formation of the APAP dimer was further confirmed by electrospray ionization mass spectrometry. Van Schepdael Ann Nève Jean Dubois Jacques Kauffmann Jean-Michel Duez Pierre Scheller Frieder Universite Libre de Bruxelles 2008-06-02 text application/pdf http://theses.ulb.ac.be/ETD-db/collection/available/ULBetd-06092008-110943/ http://theses.ulb.ac.be/ETD-db/collection/available/ULBetd-06092008-110943/ en restricted J'accepte que le texte de la thèse (ci-après l'oeuvre), sous réserve des parties couvertes par la confidentialité, soit publié dans le recueil électronique des thèses ULB. A cette fin, je donne licence à ULB : - le droit de fixer et de reproduire l'oeuvre sur support électronique : logiciel ETD/db - le droit de communiquer l'oeuvre au public Cette licence, gratuite et non exclusive, est valable pour toute la durée de la propriété littéraire et artistique, y compris ses éventuelles prolongations, et pour le monde entier. Je conserve tous les autres droits pour la reproduction et la communication de la thèse, ainsi que le droit de l'utiliser dans de futurs travaux. Je certifie avoir obtenu, conformément à la législation sur le droit d'auteur et aux exigences du droit à l'image, toutes les autorisations nécessaires à la reproduction dans ma thèse d'images, de textes, et/ou de toute oeuvre protégés par le droit d'auteur, et avoir obtenu les autorisations nécessaires à leur communication à des tiers. Au cas où un tiers est titulaire d'un droit de propriété intellectuelle sur tout ou partie de ma thèse, je certifie avoir obtenu son autorisation écrite pour l'exercice des droits mentionnés ci-dessus. |