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Potentiometric sensors based on surface molecular imprinting: Detection of cancer biomarkers and viruses

  • Stony Brook University
  • Herricks High School
  • Plainview Old Bethpage John F. Kennedy High School
  • Carnegie Institution of Washington
  • Polytechnic University

Research output: Contribution to journalArticlepeer-review

178 Scopus citations

Abstract

The continuing discovery of cancer biomarkers necessitates improved methods for their detection. Molecular imprinting using artificial materials provides an alternative to the detection of a wide range of substances. We applied surface molecular imprinting using self-assembled monolayers to design sensing elements for the detection of cancer biomarkers and other proteins. These elements consist of a gold-coated silicon chip onto which hydroxyl-terminated alkanethiol molecules and template biomolecule are co-adsorbed, where the thiol molecules are chemically bound to the metal substrate and self-assembled into highly ordered monolayers, the biomolecules can be removed, creating the foot-print cavities in the monolayer matrix for this kind of template molecules. Re-adsorption of the biomolecules to the sensing chip changes its potential, which can be measured potentiometrically. We applied this method to the detection of carcinoembryonic antigen (CEA) in both solutions of purified CEA and in the culture medium of a CEA-producing human colon cancer cell line. The CEA assay, validated also against a standard immunoassay, was both sensitive (detection range 2.5-250 ng/mL) and specific (no cross-reactivity with hemoglobin; no response by a non-imprinted sensor). Similar results were obtained for human amylase. In addition, we detected virions of poliovirus in a specific manner (no cross-reactivity to adenovirus, no response by a non-imprinted sensor). Our findings demonstrate the application of the principles of molecular imprinting to the development of a new method for the detection of protein cancer biomarkers and to protein-based macromolecular structures such as the capsid of a virion. This approach has the potential of generating a general assay methodology that could be highly sensitive, specific, simple and likely inexpensive.

Original languageEnglish
Pages (from-to)381-387
Number of pages7
JournalSensors and Actuators, B: Chemical
Volume146
Issue number1
DOIs
StatePublished - Apr 8 2010

Keywords

  • Biosensor
  • Cancer marker
  • Molecular imprinting
  • Potentiometric sensor
  • Protein recognition
  • Self-assembled monolayer

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