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Latent analysis of unmodified biomolecules and their complexes in solution with attomole detection sensitivity

机译:具有原子检测灵敏度的溶液中未修饰生物分子及其复合物的潜在分析

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摘要

The study of biomolecular interactions is central to an understanding of function, malfunction and therapeutic modulation of biological systems, yet often involves a compromise between sensitivity and accuracy. Many conventional analytical steps and the procedures required to facilitate sensitive detection, such as the incorporation of chemical labels, are prone to perturb the complexes under observation. Here we present a 'latent' analysis approach that uses chemical and microfluidic tools to reveal, through highly sensitive detection of a labelled system, the behaviour of the physiologically relevant unlabelled system. We implement this strategy in a native microfluidic diffusional sizing platform, allowing us to achieve detection sensitivity at the attomole level, determine the hydrodynamic radii of biomolecules that vary by over three orders of magnitude in molecular weight, and study heterogeneous mixtures. We illustrate these key advantages by characterizing a complex of an antibody domain in the solution phase and under physiologically relevant conditions.
机译:生物分子相互作用的研究对于了解生物系统的功能,功能失常和治疗调节至关重要,但通常会在灵敏度和准确性之间进行折衷。促进灵敏检测所需的许多常规分析步骤和程序,例如掺入化学标记,都容易干扰正在观察的络合物。在这里,我们提出一种“潜在”分析方法,该方法使用化学和微流体工具通过对标记系统的高度灵敏检测来揭示生理相关的未标记系统的行为。我们在天然的微流体扩散筛分平台上实施该策略,从而使我们能够在原子水平上实现检测灵敏度,确定分子量变化超过三个数量级的生物分子的流体动力学半径,并研究异质混合物。我们通过在溶液相和生理相关条件下表征抗体结构域的复合物来说明这些关键优势。

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