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通过仅通过优先的 DNA-底物相互作用固定的 DNA 探针实现了受控和高效的杂交。

Controlled and efficient hybridization achieved with DNA probes immobilized solely through preferential DNA-substrate interactions.

机构信息

Department of Chemistry, University of Wisconsin-La Crosse, La Crosse, Wisconsin 54601, USA.

出版信息

Anal Chem. 2010 Apr 1;82(7):2803-10. doi: 10.1021/ac902765g.

DOI:10.1021/ac902765g
PMID:20196546
Abstract

Quantitative and reproducible data can be obtained from surface-based DNA sensors if variations in the conformation and surface density of immobilized single-stranded DNA capture probes are minimized. Both the conformation and surface density can be independently and deterministically controlled by taking advantage of the preferential adsorption of adenine nucleotides (dA) on gold, as previously demonstrated using a model system in Opdahl, A.; Petrovykh, D. Y.; Kimura-Suda, H.; Tarlov, M. J.; Whitman, L. J. Proc. Natl. Acad. Sci. U.S.A. 2007, 104, 9-14. Here, we describe the immobilization and subsequent hybridization properties of a 15-nucleotide DNA probe sequence that has additional m adenine nucleotides, (dA)(m), at the 5' end. Quantitative analysis of immobilization and hybridization for these probes indicates that the (dA)(m) block preferentially adsorbs on gold, forcing the probe portion of the strand to adopt an upright conformation suited for efficient hybridization. In addition, a wide range of probe-to-probe lateral spacing can be achieved by coimmobilizing the probe DNA with a lateral spacer, a strand of k adenine nucleotides, (dA)(k). Altering either the length or relative concentration of the (dA)(k) spacers added during probe immobilization controls the average surface density of probes; the density of probes, in turn, systematically modulates their hybridization with solution targets.

摘要

如果能将固定化单链 DNA 捕获探针的构象和表面密度的变化最小化,则可以从基于表面的 DNA 传感器获得定量且可重现的数据。如 Opdahl 等人之前在模型系统中所证明的那样,通过利用腺嘌呤核苷酸 (dA) 在金上的优先吸附作用,可以独立且确定性地控制这两个构象和表面密度,A.; Petrovykh, D. Y.; Kimura-Suda, H.; Tarlov, M. J.; Whitman, L. J. Proc. Natl. Acad. Sci. U.S.A. 2007, 104, 9-14。在这里,我们描述了 15 个核苷酸 DNA 探针序列的固定化及其随后的杂交特性,该序列在 5' 端具有额外的 m 个腺嘌呤核苷酸 (dA)(m)。这些探针的固定化和杂交的定量分析表明,(dA)(m) 块优先在金上吸附,迫使链的探针部分采用适合高效杂交的直立构象。此外,通过将探针 DNA 与侧向间隔物(k 个腺嘌呤核苷酸的链,(dA)(k))共固定,可以实现探针之间的广泛的侧向间距。改变在探针固定化过程中添加的 (dA)(k) 间隔物的长度或相对浓度可以控制探针的平均表面密度;反过来,探针的密度系统地调节它们与溶液靶标的杂交。

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