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基于纳米孔的溶液中单个体淀粉样颗粒的快速表征:概念、挑战和前景。

Nanopore-Based, Rapid Characterization of Individual Amyloid Particles in Solution: Concepts, Challenges, and Prospects.

机构信息

Department of Biomedical Engineering, University of Michigan, Ann Arbor, MI, 48109, USA.

Adolphe Merkle Institute, University of Fribourg, Chemin des Verdiers 4, CH-1700, Fribourg, Switzerland.

出版信息

Small. 2018 Nov;14(46):e1802412. doi: 10.1002/smll.201802412. Epub 2018 Sep 17.

Abstract

Aggregates of misfolded proteins are associated with several devastating neurodegenerative diseases. These so-called amyloids are therefore explored as biomarkers for the diagnosis of dementia and other disorders, as well as for monitoring disease progression and assessment of the efficacy of therapeutic interventions. Quantification and characterization of amyloids as biomarkers is particularly demanding because the same amyloid-forming protein can exist in different states of assembly, ranging from nanometer-sized monomers to micrometer-long fibrils that interchange dynamically both in vivo and in samples from body fluids ex vivo. Soluble oligomeric amyloid aggregates, in particular, are associated with neurotoxic effects, and their molecular organization, size, and shape appear to determine their toxicity. This concept article proposes that the emerging field of nanopore-based analytics on a single molecule and single aggregate level holds the potential to account for the heterogeneity of amyloid samples and to characterize these particles-rapidly, label-free, and in aqueous solution-with regard to their size, shape, and abundance. The article describes the concept of nanopore-based resistive pulse sensing, reviews previous work in amyloid analysis, and discusses limitations and challenges that will need to be overcome to realize the full potential of amyloid characterization on a single-particle level.

摘要

蛋白质错误折叠的聚集体与几种严重的神经退行性疾病有关。因此,这些所谓的淀粉样蛋白被探索作为痴呆症和其他疾病的诊断标志物,以及监测疾病进展和评估治疗干预效果的标志物。作为生物标志物的淀粉样蛋白的定量和特征描述要求特别高,因为相同的淀粉样蛋白形成蛋白可能存在不同的组装状态,从纳米级的单体到微米级的原纤维,这些状态在体内和体外体液样本中都能动态地相互转化。特别是可溶性寡聚淀粉样蛋白聚集体与神经毒性有关,其分子结构、大小和形状似乎决定了其毒性。这篇概念文章提出,新兴的单分子和单聚集体水平的纳米孔分析领域有可能解释淀粉样蛋白样品的异质性,并对这些颗粒进行快速、无标记和在水溶液中的特征描述,包括其大小、形状和丰度。本文描述了基于纳米孔的电阻脉冲传感的概念,回顾了以前在淀粉样蛋白分析方面的工作,并讨论了在实现单颗粒水平的淀粉样蛋白特征描述的全部潜力方面需要克服的限制和挑战。

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