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利用多重离子淌度谱推进肝纤维化蛋白质特征的高通量鉴定。

Advancing the high throughput identification of liver fibrosis protein signatures using multiplexed ion mobility spectrometry.

作者信息

Baker Erin Shammel, Burnum-Johnson Kristin E, Jacobs Jon M, Diamond Deborah L, Brown Roslyn N, Ibrahim Yehia M, Orton Daniel J, Piehowski Paul D, Purdy David E, Moore Ronald J, Danielson William F, Monroe Matthew E, Crowell Kevin L, Slysz Gordon W, Gritsenko Marina A, Sandoval John D, Lamarche Brian L, Matzke Melissa M, Webb-Robertson Bobbie-Jo M, Simons Brenna C, McMahon Brian J, Bhattacharya Renuka, Perkins James D, Carithers Robert L, Strom Susan, Self Steven G, Katze Michael G, Anderson Gordon A, Smith Richard D

机构信息

Biological Sciences Division and Environmental Molecular Sciences Laboratory, Pacific Northwest National Laboratory, Richland, Washington;

出版信息

Mol Cell Proteomics. 2014 Apr;13(4):1119-27. doi: 10.1074/mcp.M113.034595. Epub 2014 Jan 8.

Abstract

Rapid diagnosis of disease states using less invasive, safer, and more clinically acceptable approaches than presently employed is a crucial direction for the field of medicine. While MS-based proteomics approaches have attempted to meet these objectives, challenges such as the enormous dynamic range of protein concentrations in clinically relevant biofluid samples coupled with the need to address human biodiversity have slowed their employment. Herein, we report on the use of a new instrumental platform that addresses these challenges by coupling technical advances in rapid gas phase multiplexed ion mobility spectrometry separations with liquid chromatography and MS to dramatically increase measurement sensitivity and throughput, further enabling future high throughput MS-based clinical applications. An initial application of the liquid chromatography--ion mobility spectrometry-MS platform analyzing blood serum samples from 60 postliver transplant patients with recurrent fibrosis progression and 60 nontransplant patients illustrates its potential utility for disease characterization.

摘要

使用比目前所采用的方法侵入性更小、更安全且在临床上更易接受的方法来快速诊断疾病状态,是医学领域的一个关键方向。虽然基于质谱的蛋白质组学方法试图实现这些目标,但诸如临床相关生物流体样本中蛋白质浓度的巨大动态范围,以及应对人类生物多样性的需求等挑战,减缓了它们的应用。在此,我们报告了一种新的仪器平台的使用情况,该平台通过将快速气相多路复用离子迁移谱分离技术的进展与液相色谱和质谱相结合,来应对这些挑战,从而显著提高测量灵敏度和通量,进一步推动未来基于质谱的高通量临床应用。液相色谱-离子迁移谱-质谱平台对60例肝移植后复发性纤维化进展患者和60例非移植患者的血清样本进行分析的初步应用,说明了其在疾病特征描述方面的潜在效用。

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