Ternary monolayers as DNA recognition interfaces for direct and sensitive electrochemical detection in untreated clinical samples

Detection of specific DNA sequences in clinical samples is a key goal of studies on DNA biosensors and gene chips. Herein we present a highly sensitive electrochemical genosensor for direct measurements of specific DNA sequences in undiluted and untreated human serum and urine samples. Such genosens...

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Published inBiosensors & bioelectronics Vol. 26; no. 8; pp. 3577 - 3583
Main Authors Campuzano, Susana, Kuralay, Filiz, Lobo-Castañón, M. Jesús, Bartošík, Martin, Vyavahare, Kedar, Paleček, Emil, Haake, David A., Wang, Joseph
Format Journal Article
LanguageEnglish
Published Kidlington Elsevier B.V 15.04.2011
Elsevier
Subjects
Biological and medical sciences
Biosensing Techniques - methods
Biotechnology
Clinical samples
Dithiols
DNA
DNA - analysis
Electrochemical detection
Electrochemical Techniques
Fundamental and applied biological sciences. Psychology
Humans
Hybridization
Self-assembled monolayer
Self-assembled monolayer
Clinical samples
Electrochemical detection
Hybridization
Dithiols
DNA
Self assembly
Monolayer
Sample
Electrochemistry
Detection
Recognition
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Summary:Detection of specific DNA sequences in clinical samples is a key goal of studies on DNA biosensors and gene chips. Herein we present a highly sensitive electrochemical genosensor for direct measurements of specific DNA sequences in undiluted and untreated human serum and urine samples. Such genosensing relies on a new ternary interface involving hexanedithiol (HDT) co-immobilized with the thiolated capture probe (SHCP) on gold surfaces, followed by the incorporation of 6-mercapto-1-hexanol (MCH) as diluent. The performance of ternary monolayers prepared with linear dithiols of different lengths was systematically examined, compared and characterized by cyclic voltammetry and electrochemical impedance spectroscopy, with HDT exhibiting the most favorable analytical performance. The new SHCP/HDT + MCH monolayer led to a 80-fold improvement in the signal-to-noise ratio (S/N) for 1 nM target DNA in undiluted human serum over the common SHCP+MCH binary alkanethiol interface, and allowed the direct quantification of the target DNA down to 7 pM (28 amol) and 17 pM (68 amol) in undiluted/untreated serum and urine, respectively. It also displayed attractive antifouling properties, as indicated from the favorable S/N obtained after a prolonged exposure (24 h) to untreated biological matrices. These attractive features of the SHCP/HDT + MCH sensor interface indicate considerable promise for a wide range of clinical applications.
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ISSN:0956-5663
1873-4235
DOI:10.1016/j.bios.2011.02.004