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基于三螺旋分子开关的适体传感平台的设计。

Design of aptamer-based sensing platform using triple-helix molecular switch.

机构信息

State Key Laboratory of Chemo/Biosensing and Chemometrics, College of Chemistry and Chemical Engineering, Hunan University, Changsha, 410082, China.

出版信息

Anal Chem. 2011 Sep 1;83(17):6586-92. doi: 10.1021/ac201314y. Epub 2011 Aug 12.

Abstract

For successful assay development of an aptamer-based biosensor, various design principles and strategies, including a highly selective molecular recognition element and a novel signal transduction mechanism, have to be engineered together. Herein, we report a new type of aptamer-based sensing platform which is based on a triple-helix molecular switch (THMS). The THMS consists of a central, target specific aptamer sequence flanked by two arm segments and a dual-labeled oligonucleotide serving as a signal transduction probe (STP). The STP is doubly labeled with pyrene at the 5'- and 3'-end, respectively, and initially designed as a hairpin-shaped structure, thus, bringing the two pyrenes into spacer proximity. Bindings of two arm segments of the aptamer with the loop sequence of STP enforce the STP to form an "open" configuration. Formation of aptamer/target complex releases the STP, leading to new signal readout. To demonstrate the feasibility and universality of our design, three aptamers which bind to human α-thrombin (Tmb), adenosine triphosphate (ATP), and L-argininamide (L-Arm), respectively, were selected as models. The universality of the approach is achieved by virtue of altering the aptamer sequence without change of the triple-helix structure.

摘要

为了成功开发基于适配体的生物传感器的分析方法,必须将各种设计原则和策略结合在一起,包括高度选择性的分子识别元件和新型信号转导机制。在此,我们报告了一种基于三螺旋分子开关 (THMS) 的新型适配体传感平台。THMS 由中央靶特异性适配体序列两侧的两个臂段和作为信号转导探针 (STP) 的双标记寡核苷酸组成。STP 在 5' 和 3' 末端分别用芘标记,最初设计为发夹状结构,从而使两个芘进入间隔接近。适配体的两个臂段与 STP 的环序列的结合迫使 STP 形成“打开”构型。适配体/靶复合物的形成释放 STP,导致新的信号读出。为了证明我们设计的可行性和通用性,选择了分别与人凝血酶 (Tmb)、三磷酸腺苷 (ATP) 和 L-精氨酰胺 (L-Arm) 结合的三种适配体作为模型。通过改变适配体序列而不改变三螺旋结构来实现方法的通用性。

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