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用于表征纳米材料获得的蛋白质和代谢物冠层的毛细管电泳质谱方法。

Capillary Electrophoresis Mass Spectrometry Approaches for Characterization of the Protein and Metabolite Corona Acquired by Nanomaterials.

作者信息

Chetwynd Andrew J, Zhang Wei, Faserl Klaus, Thorn James A, Lynch Iseult, Ramautar Rawi, Lindner Herbert H

机构信息

School of Geography Earth and Environmental Sciences, University of Birmingham;

Biomedical Microscale Analytics, Leiden University.

出版信息

J Vis Exp. 2020 Oct 27(164). doi: 10.3791/61760.

Abstract

The adsorption of biomolecules from surrounding biological matrices to the surface of nanomaterials (NMs) to form the corona has been of interest for the past decade. Interest in the bio-nano interface arises from the fact that the biomolecular corona confers a biological identity to NMs and thus causes the body to identify them as "self". For example, previous studies have demonstrated that the proteins in the corona are capable of interacting with membrane receptors to influence cellular uptake and established that the corona is responsible for cellular trafficking of NMs and their eventual toxicity. To date, most research has focused upon the protein corona and overlooked the possible impacts of the metabolites included in the corona or synergistic effects between components in the complete biomolecular corona. As such, this work demonstrates methodologies to characterize both the protein and metabolite components of the biomolecular corona using bottom-up proteomics and metabolomics approaches in parallel. This includes an on-particle digest of the protein corona with a surfactant used to increase protein recovery, and a passive characterization of the metabolite corona by analyzing metabolite matrices before and after NM exposures. This work introduces capillary electrophoresis - mass spectrometry (CESI-MS) as a new technique for NM corona characterization. The protocols outlined here demonstrate how CESI-MS can be used for the reliable characterization of both the protein and metabolite corona acquired by NMs. The move to CESI-MS greatly decreases the volume of sample required (compared to traditional liquid chromatography - mass spectrometry (LC-MS) approaches) with multiple injections possible from as little as 5 µL of sample, making it ideal for volume limited samples. Furthermore, the environmental consequences of analysis are reduced with respect to LC-MS due to the low flow rates (<20 nL/min) in CESI-MS, and the use of aqueous electrolytes which eliminates the need for organic solvents.

摘要

在过去十年中,生物分子从周围生物基质吸附到纳米材料(NMs)表面形成冠层一直备受关注。对生物-纳米界面的兴趣源于生物分子冠层赋予纳米材料生物特性,从而使机体将它们识别为“自身”这一事实。例如,先前的研究表明,冠层中的蛋白质能够与膜受体相互作用以影响细胞摄取,并确定冠层负责纳米材料的细胞转运及其最终毒性。迄今为止,大多数研究都集中在蛋白质冠层上,而忽略了冠层中所含代谢物的可能影响或完整生物分子冠层中各成分之间的协同效应。因此,这项工作展示了使用自下而上的蛋白质组学和代谢组学方法并行表征生物分子冠层的蛋白质和代谢物成分的方法。这包括用一种用于提高蛋白质回收率的表面活性剂对蛋白质冠层进行颗粒上消化,以及通过分析纳米材料暴露前后的代谢物基质对代谢物冠层进行被动表征。这项工作引入了毛细管电泳-质谱联用(CESI-MS)作为一种用于纳米材料冠层表征的新技术。这里概述的方案展示了CESI-MS如何用于可靠地表征纳米材料获得的蛋白质和代谢物冠层。转向CESI-MS极大地减少了所需样品的体积(与传统液相色谱-质谱联用(LC-MS)方法相比),只需5微升样品就可以进行多次进样,使其非常适合样品量有限的情况。此外,由于CESI-MS的流速较低(<20纳升/分钟),并且使用水性电解质从而无需有机溶剂,与LC-MS相比,分析对环境的影响更小。

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