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Dynamic Isolation and Unloading of Target Proteins by Aptamer-Modified Microtransporters

机译:通过适配体修饰的微转运蛋白动态分离和卸载靶蛋白

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摘要

We describe here a new strategy for isolating target proteins from complex biological samples based on an aptamer-modified self-propelled microtube engine. For this purpose, a thiolated thrombin or a mixed thrombin-ATP aptamer (prehybridized with a thiolated short DNA) was coassembled with mercaptohexanol onto the gold surface of these microtube engines. The rapid movement of the aptamer-modified microtransporter resulted in highly selective and rapid capture of the target thrombin, with an effective discrimination against a large excess of nontarget proteins. Release of the captured thrombin can be triggered by the addition of ATP that can bind and displace the immobilized mixed thrombin-ATP aptamer in 20 min. The rapid loading and unloading abilities demonstrated by these selective microtransporters are illustrated in complex matrixes such as human serum and plasma. The new motion-driven protein isolation platform represents a new approach in bioanalytical chemistry based on active transport of proteins and offers considerable promise for diverse diagnostic applications.
机译:我们在这里描述了一种基于适配体修饰的自走式微管发动机从复杂生物样品中分离靶蛋白的新策略。为此,将硫醇化凝血酶或混合凝血酶-ATP适配体(与硫醇化短DNA预杂交)与巯基己醇共组装到这些微管发动机的金表面上。适配体修饰的微转运蛋白的快速移动导致对靶凝血酶的高选择性和快速捕获,并有效区分大量过量的非靶蛋白。捕获的凝血酶的释放可以通过添加ATP来触发,ATP可以在20分钟内结合并置换固定的混合凝血酶-ATP适配体。这些选择性微转运蛋白所表现出的快速上样和卸载能力在复杂的基质(如人血清和血浆)中得到了说明。新的运动驱动蛋白质分离平台代表了一种基于蛋白质主动转运的生物分析化学新方法,并为各种诊断应用提供了相当大的前景。

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