Enhanced Biosensor Platforms for Detecting the Atherosclerotic Biomarker VCAM1 Based on Bioconjugation with Uniformly Oriented VCAM1-Targeting Nanobodies

Surface bioconjugation of biomolecules has gained enormous attention for developing advanced biomaterials including biosensors. While conventional immobilization (by physisorption or covalent couplings using the functional groups of the endogenous amino acids) usually results in surfaces with low ac...

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Main Authors: Duy Tien Ta, Wanda Guedens, Tom Vranken, Katrijn Vanschoenbeek, Erik Steen Redeker, Luc Michiels, Peter Adriaensens
Format: Article
Language:English
Published: MDPI AG 2016-07-01
Series:Biosensors
Subjects:
Online Access:http://www.mdpi.com/2079-6374/6/3/34
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spelling doaj-ab3902c6b49a4d7cb5dd3c206eead7302020-11-24T22:08:58ZengMDPI AGBiosensors2079-63742016-07-01633410.3390/bios6030034bios6030034Enhanced Biosensor Platforms for Detecting the Atherosclerotic Biomarker VCAM1 Based on Bioconjugation with Uniformly Oriented VCAM1-Targeting NanobodiesDuy Tien Ta0Wanda Guedens1Tom Vranken2Katrijn Vanschoenbeek3Erik Steen Redeker4Luc Michiels5Peter Adriaensens6Biomolecule Design Group, Institute for Materials Research (IMO), Hasselt University, Diepenbeek BE-3590, BelgiumBiomolecule Design Group, Institute for Materials Research (IMO), Hasselt University, Diepenbeek BE-3590, BelgiumBiomolecule Design Group, Institute for Materials Research (IMO), Hasselt University, Diepenbeek BE-3590, BelgiumImmunology and Biochemistry, Biomedical Research Institute (Biomed) and School of Life Sciences, Transnationale Universiteit Limburg, Hasselt University, Diepenbeek BE-3590, BelgiumMaastricht Science Programme, Maastricht University, Maastricht 6200 MD, The NetherlandsImmunology and Biochemistry, Biomedical Research Institute (Biomed) and School of Life Sciences, Transnationale Universiteit Limburg, Hasselt University, Diepenbeek BE-3590, BelgiumBiomolecule Design Group, Institute for Materials Research (IMO), Hasselt University, Diepenbeek BE-3590, BelgiumSurface bioconjugation of biomolecules has gained enormous attention for developing advanced biomaterials including biosensors. While conventional immobilization (by physisorption or covalent couplings using the functional groups of the endogenous amino acids) usually results in surfaces with low activity, reproducibility and reusability, the application of methods that allow for a covalent and uniformly oriented coupling can circumvent these limitations. In this study, the nanobody targeting Vascular Cell Adhesion Molecule-1 (NbVCAM1), an atherosclerotic biomarker, is engineered with a C-terminal alkyne function via Expressed Protein Ligation (EPL). Conjugation of this nanobody to azidified silicon wafers and Biacore™ C1 sensor chips is achieved via Copper(I)-catalyzed azide-alkyne cycloaddition (CuAAC) “click” chemistry to detect VCAM1 binding via ellipsometry and surface plasmon resonance (SPR), respectively. The resulting surfaces, covered with uniformly oriented nanobodies, clearly show an increased antigen binding affinity, sensitivity, detection limit, quantitation limit and reusability as compared to surfaces prepared by random conjugation. These findings demonstrate the added value of a combined EPL and CuAAC approach as it results in strong control over the surface orientation of the nanobodies and an improved detecting power of their targets—a must for the development of advanced miniaturized, multi-biomarker biosensor platforms.http://www.mdpi.com/2079-6374/6/3/34uniformly oriented bioconjugationbiosensorCuAACexpressed protein ligationVCAM1-targeting nanobody
collection DOAJ
language English
format Article
sources DOAJ
author Duy Tien Ta
Wanda Guedens
Tom Vranken
Katrijn Vanschoenbeek
Erik Steen Redeker
Luc Michiels
Peter Adriaensens
spellingShingle Duy Tien Ta
Wanda Guedens
Tom Vranken
Katrijn Vanschoenbeek
Erik Steen Redeker
Luc Michiels
Peter Adriaensens
Enhanced Biosensor Platforms for Detecting the Atherosclerotic Biomarker VCAM1 Based on Bioconjugation with Uniformly Oriented VCAM1-Targeting Nanobodies
Biosensors
uniformly oriented bioconjugation
biosensor
CuAAC
expressed protein ligation
VCAM1-targeting nanobody
author_facet Duy Tien Ta
Wanda Guedens
Tom Vranken
Katrijn Vanschoenbeek
Erik Steen Redeker
Luc Michiels
Peter Adriaensens
author_sort Duy Tien Ta
title Enhanced Biosensor Platforms for Detecting the Atherosclerotic Biomarker VCAM1 Based on Bioconjugation with Uniformly Oriented VCAM1-Targeting Nanobodies
title_short Enhanced Biosensor Platforms for Detecting the Atherosclerotic Biomarker VCAM1 Based on Bioconjugation with Uniformly Oriented VCAM1-Targeting Nanobodies
title_full Enhanced Biosensor Platforms for Detecting the Atherosclerotic Biomarker VCAM1 Based on Bioconjugation with Uniformly Oriented VCAM1-Targeting Nanobodies
title_fullStr Enhanced Biosensor Platforms for Detecting the Atherosclerotic Biomarker VCAM1 Based on Bioconjugation with Uniformly Oriented VCAM1-Targeting Nanobodies
title_full_unstemmed Enhanced Biosensor Platforms for Detecting the Atherosclerotic Biomarker VCAM1 Based on Bioconjugation with Uniformly Oriented VCAM1-Targeting Nanobodies
title_sort enhanced biosensor platforms for detecting the atherosclerotic biomarker vcam1 based on bioconjugation with uniformly oriented vcam1-targeting nanobodies
publisher MDPI AG
series Biosensors
issn 2079-6374
publishDate 2016-07-01
description Surface bioconjugation of biomolecules has gained enormous attention for developing advanced biomaterials including biosensors. While conventional immobilization (by physisorption or covalent couplings using the functional groups of the endogenous amino acids) usually results in surfaces with low activity, reproducibility and reusability, the application of methods that allow for a covalent and uniformly oriented coupling can circumvent these limitations. In this study, the nanobody targeting Vascular Cell Adhesion Molecule-1 (NbVCAM1), an atherosclerotic biomarker, is engineered with a C-terminal alkyne function via Expressed Protein Ligation (EPL). Conjugation of this nanobody to azidified silicon wafers and Biacore™ C1 sensor chips is achieved via Copper(I)-catalyzed azide-alkyne cycloaddition (CuAAC) “click” chemistry to detect VCAM1 binding via ellipsometry and surface plasmon resonance (SPR), respectively. The resulting surfaces, covered with uniformly oriented nanobodies, clearly show an increased antigen binding affinity, sensitivity, detection limit, quantitation limit and reusability as compared to surfaces prepared by random conjugation. These findings demonstrate the added value of a combined EPL and CuAAC approach as it results in strong control over the surface orientation of the nanobodies and an improved detecting power of their targets—a must for the development of advanced miniaturized, multi-biomarker biosensor platforms.
topic uniformly oriented bioconjugation
biosensor
CuAAC
expressed protein ligation
VCAM1-targeting nanobody
url http://www.mdpi.com/2079-6374/6/3/34
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