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首页> 外文期刊>Nanoscale >Glutathione-functionalized magnetic thioether-COFs for the simultaneous capture of urinary exosomes and enrichment of exosomal glycosylated and phosphorylated peptides
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Glutathione-functionalized magnetic thioether-COFs for the simultaneous capture of urinary exosomes and enrichment of exosomal glycosylated and phosphorylated peptides

机译:Glutathione-functionalized磁thioether-COFs同时捕获的尿液和浓缩exosomal糖化和磷酸化肽

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摘要

Exosomes play an irreplaceable role in physiological and pathological processes, and the study of proteomics (especially protein post-translational modifications, PTMs) in exosomes can reveal the pathogenesis of diseases and screen therapeutic disease targets. The separation and enrichment process is an essential step in mass spectroscopy-based exosomal PTMs studies to reduce sample complexity and ionization-suppression effects. Herein, we designed a novel magnetic zwitterionic material, namely glutathione-functionalized thioether covalent organic frameworks (Fe3O4@Thio-COF@Au@GSH), possessing fast magnetic responsiveness, regular porosity, and a suitable surface area. Thanks to the hydrophilicity and charge-switchable feature of GSH, for the first time, both the capture of exosomes from biological fluids and enrichment of the inherent glycoproteins/phosphoproteins in the exosomes were achieved with the same material. Furthermore, the high enrichment capacity was validated by theoretical calculations. The low detection limits (0.2/0.4 fmol for HRP/β-casein), high selectivity (1 : 1000 for HRP/β-casein : BSA molar ratio), and high exosomal glycoproteomics/phosphoproteomics profiling capability proved the feasibility of the developed method. This work provides a new heuristic strategy to solve the problems of exosomal capture and glycoproteins/phosphoproteins pretreatment in exosomal proteomics.
机译:液中发挥着不可替代的作用生理和病理过程,蛋白质组学的研究(尤其是蛋白质转录后修饰,天车)液可以揭示疾病的发病机理和屏幕治疗疾病的目标。分离和浓缩过程是必不可少的一步质量spectroscopy-based exosomal天车研究减少复杂性和示例ionization-suppression效果。设计了一种新型磁两性离子材料,即glutathione-functionalized硫醚共价有机框架(Fe3O4@Thio-COF@Au@GSH),拥有快速磁响应性,常规孔隙度、和一个合适的表面积。谷胱甘肽的charge-switchable特性,第一液的捕获时间生物体液和固有的浓缩糖蛋白在液/磷蛋白质是用同样的材料来实现。此外,高浓缩能力验证了理论计算。检测极限(0.2/0.4 fmol合/β酪蛋白),高选择性(1:1000年合/β酪蛋白:BSA摩尔比),和高exosomalglycoproteomics / phosphoproteomics剖析能力证明的可行性开发的方法。启发式策略来解决的问题exosomal捕获和糖蛋白/磷蛋白质预处理exosomal蛋白质组学。

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