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Immobilization of aptamers onto unmodified glass surfaces for affordable biosensors

机译:将适体固定在未经修饰的玻璃表面上,以实现可负担的生物传感器

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Silicon dioxide surfaces are commonly used in photonic microsensors for bioreceptor attachment. Functionalization of sensor surface with aptamer receptors provides the opportunity to develop low cost, robust, field deployable sensors. Most aptamer sensors are constructed by covalently linking modified aptamers to a derivatized surface. There have been reports of using UV crosslinking to directly immobilize DNA with sequences that end with poly(T)10-poly(C)10 on an unmodified glass surface for hybridization. We have expanded this strategy using thrombin-binding aptamers (TBAs) with three different tail modifications. TBA with PolyT20 tail showed the best performance in terms of sensitivity and dynamic range. PolyTC tailed aptamers did not bind thrombin well, which may be due to that the interactions between the C bases and G-quadruplex affect their target binding capability. When compared to biotinylated aptamer immobilized on a streptavidin surface, polyT aptamer printed directly on plain glass showed comparable affinity. Direct immobilization of TBA on nonfunctionalized silicon dioxide wafer and its binding towards thrombin has also been demonstrated. Our results showed that using polyT-tagged aptamer probes directly immobilized on unmodified glass and SiO2 surface is a robust, very straightforward, and inexpensive method for preparing biosensors
机译:二氧化硅表面通常用于光子微传感器中的生物受体附着。带有适体受体的传感器表面功能化提供了开发低成本,坚固,可现场部署的传感器的机会。大多数适体传感器是通过将修饰的适体共价连接到衍生化的表面而构建的。已经有报道使用UV交联直接将DNA序列固定在未修饰的玻璃表面上的以poly(T)10-poly(C)10结尾的DNA进行杂交。我们已使用具有三种不同尾部修饰的凝血酶结合适体(TBA)扩展了该策略。带有PolyT20尾部的TBA在灵敏度和动态范围方面显示出最佳性能。 PolyTC尾部的适体不能很好地结合凝血酶,这可能是由于C碱基和G-四链体之间的相互作用影响了它们的靶结合能力。与固定在链霉亲和素表面上的生物素化适体相比,直接印刷在普通玻璃上的polyT适体表现出可比的亲和力。还已经证明了将TBA直接固定在未官能化的二氧化硅晶片上及其与凝血酶的结合。我们的结果表明,使用直接固定在未修饰的玻璃和SiO2表面上的polyT标签适体探针是一种制备生物传感器的可靠,非常直接且便宜的方法

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