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Nanotube–antibody biosensor arrays for the detection of circulating breast cancer cells

Ning Shao1, Eric Wickstrom2,3 and Balaji Panchapakesan1,4

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Recent reports have shown that nanoscale electronic devices can be used to detect a change in electrical properties when receptor proteins bind to their corresponding antibodies functionalized on the surface of the device, in extracts from as few as ten lysed tumor cells. We hypothesized that nanotube–antibody devices could sensitively and specifically detect entire live cancer cells. We report for the first time a single nanotube field effect transistor array, functionalized with IGF1R-specific and Her2-specific antibodies, which exhibits highly sensitive and selective sensing of live, intact MCF7 and BT474 human breast cancer cells in human blood. Those two cell lines both overexpress IGF1R and Her2, at different levels. Single or small bundle of nanotube devices that were functionalized with IGF1R-specific or Her2-specific antibodies showed 60% decreases in conductivity upon interaction with BT474 or MCF7 breast cancer cells in two µl drops of blood. Control experiments with non-specific antibodies or with MCF10A control breast cells produced a less than 5% decrease in electrical conductivity, illustrating the high sensitivity for whole cell binding by these single nanotube–antibody devices. We postulate that the free energy change due to multiple simultaneous cell–antibody binding events exerted stress along the nanotube surface, decreasing its electrical conductivity due to an increase in band gap. Because the free energy change upon cell–antibody binding, the stress exerted on the nanotube, and the change in conductivity are specific to a specific antigen–antibody interaction; these properties might be used as a fingerprint for the molecular sensing of circulating cancer cells. From optical microscopy observations during sensing, it appears that the binding of a single cell to a single nanotube field effect transistor produced the change in electrical conductivity. Thus we report a nanoscale oncometer with single cell sensitivity with a diameter 1000 times smaller than a cancer cell that functions in a drop of fresh blood.


PACS

87.85.Qr Nanotechnologies-design

85.35.Kt Nanotube devices

87.14.E- Proteins

87.19.X- Diseases

87.19.U- Hemodynamics

87.15.K- Molecular interactions; membrane-protein interactions

Subjects

Electronics and devices

Medical physics

Biological physics

Nanoscale science and low-D systems

Dates

Issue 46 (19 November 2008)

Received 20 May 2008, in final form 16 August 2008

Published 21 October 2008



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    Ning Shao et al 2008 Nanotechnology 19 465101

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