Issue 3, 2008

Single-molecule detection of DNAvia sequence-specific links between F1-ATPase motors and gold nanorod sensors

Abstract

We report the construction of a novel biosensing nanodevice to detect single, sequence-specific target DNA molecules. Nanodevice assembly occurs through the association of an immobilized F1-ATPase molecular motor and a functionalized gold nanorodvia a single 3′,5′-dibiotinylated DNA molecule. Target-dependent 3′,5′-dibiotinylated DNA bridges form by combining ligation and exonucleation reactions (LXR), with a specificity capable of selecting against a single nucleotide polymorphism (SNP). Using dark field microscopy to detect gold nanorods, quantitation of assembled nanodevices is sufficient to distinguish the presence of as few as 1800 DNA bridges from nonspecifically bound nanorods. The rotary mechanism of F1-ATPase can drive gold nanorod rotation when the nanorod is attached via the DNA bridge. Therefore, rotation discriminates fully assembled devices from nonspecifically bound nanorods, resulting in a sensitivity limit of one zeptomole (600 molecules).

Graphical abstract: Single-molecule detection of DNAvia sequence-specific links between F1-ATPase motors and gold nanorod sensors

Supplementary files

Article information

Article type
Paper
Submitted
30 Oct 2007
Accepted
18 Dec 2007
First published
07 Feb 2008

Lab Chip, 2008,8, 415-419

Single-molecule detection of DNAvia sequence-specific links between F1-ATPase motors and gold nanorod sensors

J. York, D. Spetzler, F. Xiong and W. D. Frasch, Lab Chip, 2008, 8, 415 DOI: 10.1039/B716744J

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