Electrochemical Biosensors - Sensor Principles and Architectures
Abstract
:1. Introduction
- The biocatalyst must be highly specific for the purpose of the analysis, be stable under normal storage conditions and show a low variation between assays.
- The reaction should be as independent as manageable of such physical parameters as stirring, pH and temperature. This will allow analysis of samples with minimal pre-treatment. If the reaction involves cofactors or coenzymes these should, preferably, also be co-immobilized with the enzyme.
- The response should be accurate, precise, reproducible and linear over the concentration range of interest, without dilution or concentration. It should also be free from electrical or other transducer induced noise.
- If the biosensor is to be used for invasive monitoring in clinical situations, the probe must be tiny and biocompatible, having no toxic or antigenic effects. Furthermore, the biosensor should not be prone to inactivation or proteolysis.
- For rapid measurements of analytes from human samples it is desirable that the biosensor can provide real-time analysis.
- The complete biosensor should be cheap, small, portable and capable of being used by semi-skilled operators.
2. Devices
2.1. Electrochemical Detection Techniques
2.1.1. Cyclic Voltammetry (CV)
2.1.2. Chronoamperometry and Chronopotentiometry
2.1.3. Electrochemical Impedance Spectroscopy (EIS)
2.1.4. Field-Effect Transistor (FET)
2.2. Nanowires
2.3. Electrochemistry in Combination with Complementary Biosensor Techniques
2.3.1. Electrochemical Surface-Plasmon Resonance (EC-SPR)
2.3.2. Waveguide-Based Techniques and Electrochemistry
2.3.3. Ellipsometry and Electrochemistry
2.3.4. Electrochemical Quartz Crystal Microbalance with Dissipation monitoring (EC-QCM-D)
2.3.5. Scanning Probe Microscopy (SPM)
2.4. Magnetic Biosensors
3. Surface Architecture
3.1. Surface Materials and Modifications
3.2. Electrochemical Signal Transduction
3.3. Enzymes
3.4. Recognition Elements
3.4.1. Antibodies
3.4.2. Antibody Fragments
3.4.3. Aptamers
3.5. Encapsulation of Enzymes
3.5.1. Polyelectrolyte Multilayer (PEM) Capsules
3.5.2. Vesicles
3.5.3. Polymeric Micelles
3.5.4. Hydrogel
3.5.5. Sol-Gel
3.6. Supported Lipid Bilayer Sensor Architectures
4. Conclusions & Outlook
Acknowledgments
References
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Grieshaber, D.; MacKenzie, R.; Vörös, J.; Reimhult, E. Electrochemical Biosensors - Sensor Principles and Architectures. Sensors 2008, 8, 1400-1458. https://doi.org/10.3390/s80314000
Grieshaber D, MacKenzie R, Vörös J, Reimhult E. Electrochemical Biosensors - Sensor Principles and Architectures. Sensors. 2008; 8(3):1400-1458. https://doi.org/10.3390/s80314000
Chicago/Turabian StyleGrieshaber, Dorothee, Robert MacKenzie, Janos Vörös, and Erik Reimhult. 2008. "Electrochemical Biosensors - Sensor Principles and Architectures" Sensors 8, no. 3: 1400-1458. https://doi.org/10.3390/s80314000