Mismatch detection in DNA monolayers by atomic force microscopy and electrochemical impedance spectroscopy

Maryse D. Nkoua Ngavouka; Pietro Capaldo; Elena Ambrosetti; Giacinto Scoles; Loredana Casalis; Pietro Parisse

doi:10.3762/bjnano.7.20

Beilstein Journal of Nanotechnology (Feb 2016)

Mismatch detection in DNA monolayers by atomic force microscopy and electrochemical impedance spectroscopy

Maryse D. Nkoua Ngavouka,
Pietro Capaldo,
Elena Ambrosetti,
Giacinto Scoles,
Loredana Casalis,
Pietro Parisse

Affiliations

Maryse D. Nkoua Ngavouka: Elettra-Sincrotrone Trieste S.C.p.A., s.s. 14 km 163.5 in Area Science Park, Basovizza, Trieste, Italy
Pietro Capaldo: Elettra-Sincrotrone Trieste S.C.p.A., s.s. 14 km 163.5 in Area Science Park, Basovizza, Trieste, Italy
Elena Ambrosetti: Elettra-Sincrotrone Trieste S.C.p.A., s.s. 14 km 163.5 in Area Science Park, Basovizza, Trieste, Italy
Giacinto Scoles: Department of Medical and Biological Sciences, University of Udine, Udine, Italy
Loredana Casalis: Elettra-Sincrotrone Trieste S.C.p.A., s.s. 14 km 163.5 in Area Science Park, Basovizza, Trieste, Italy
Pietro Parisse: Elettra-Sincrotrone Trieste S.C.p.A., s.s. 14 km 163.5 in Area Science Park, Basovizza, Trieste, Italy

DOI: https://doi.org/10.3762/bjnano.7.20
Journal volume & issue: Vol. 7, no. 1
pp. 220 – 227

Abstract

Read online

Background: DNA hybridization is at the basis of most current technologies for genotyping and sequencing, due to the unique properties of DNA base-pairing that guarantee a high grade of selectivity. Nonetheless the presence of single base mismatches or not perfectly matched sequences can affect the response of the devices and the major challenge is, nowadays, to distinguish a mismatch of a single base and, at the same time, unequivocally differentiate devices read-out of fully and partially matching sequences.Results: We present here two platforms based on different sensing strategies, to detect mismatched and/or perfectly matched complementary DNA strands hybridization into ssDNA oligonucleotide monolayers. The first platform exploits atomic force microscopy-based nanolithography to create ssDNA nano-arrays on gold surfaces. AFM topography measurements then monitor the variation of height of the nanostructures upon biorecognition and then follow annealing at different temperatures. This strategy allowed us to clearly detect the presence of mismatches. The second strategy exploits the change in capacitance at the interface between an ssDNA-functionalized gold electrode and the solution due to the hybridization process in a miniaturized electrochemical cell. Through electrochemical impedance spectroscopy measurements on extended ssDNA self-assembled monolayers we followed in real-time the variation of capacitance, being able to distinguish, through the difference in hybridization kinetics, not only the presence of single, double or triple mismatches in the complementary sequence, but also the position of the mismatched base pair with respect to the electrode surface.Conclusion: We demonstrate here two platforms based on different sensing strategies as sensitive and selective tools to discriminate mismatches. Our assays are ready for parallelization and can be used in the detection and quantification of single nucleotide mismatches in microRNAs or in genomic DNA.

Published in Beilstein Journal of Nanotechnology

ISSN: 2190-4286 (Online)
Publisher: Beilstein-Institut
Country of publisher: Germany
LCC subjects: Technology: Chemical technology; Science: Physics
Website: http://www.beilstein-journals.org/bjnano/home/home.htm

About the journal

Abstract

Keywords