A Calibration Method for Nanowire Biosensors to Suppress Device-to-Device Variation

Nanowire/nanotube biosensors have stimulated significant interest; however, the inevitable device-to-device variation in the biosensor performance remains a great challenge. We have developed an analytical method to calibrate nanowire biosensor responses that can suppress the device-to-device variat...

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Veröffentlicht in:ACS nano 2009-12, Vol.3 (12), p.3969-3976
Hauptverfasser: Ishikawa, Fumiaki N, Curreli, Marco, Chang, Hsiao-Kang, Chen, Po-Chiang, Zhang, Rui, Cote, Richard J, Thompson, Mark E, Zhou, Chongwu
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Sprache:eng
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Zusammenfassung:Nanowire/nanotube biosensors have stimulated significant interest; however, the inevitable device-to-device variation in the biosensor performance remains a great challenge. We have developed an analytical method to calibrate nanowire biosensor responses that can suppress the device-to-device variation in sensing response significantly. The method is based on our discovery of a strong correlation between the biosensor gate dependence (dI ds/dV g) and the absolute response (absolute change in current, ΔI). In2O3 nanowire-based biosensors for streptavidin detection were used as the model system. Studying the liquid gate effect and ionic concentration dependence of strepavidin sensing indicates that electrostatic interaction is the dominant mechanism for sensing response. Based on this sensing mechanism and transistor physics, a linear correlation between the absolute sensor response (ΔI) and the gate dependence (dI ds/dV g) is predicted and confirmed experimentally. Using this correlation, a calibration method was developed where the absolute response is divided by dI ds/dV g for each device, and the calibrated responses from different devices behaved almost identically. Compared to the common normalization method (normalization of the conductance/resistance/current by the initial value), this calibration method was proven advantageous using a conventional transistor model. The method presented here substantially suppresses device-to-device variation, allowing the use of nanosensors in large arrays.
ISSN:1936-0851
1936-086X
DOI:10.1021/nn9011384