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血浆蛋白质组和肽组的基质辅助激光解吸电离飞行时间质谱图。

The MALDI-TOF mass spectrometric view of the plasma proteome and peptidome.

作者信息

Hortin Glen L

机构信息

Department of Laboratory Medicine, National Institutes of Health, Bldg 10, Room 2C-407, Bethesda, MD 20892, USA.

出版信息

Clin Chem. 2006 Jul;52(7):1223-37. doi: 10.1373/clinchem.2006.069252. Epub 2006 Apr 27.

Abstract

BACKGROUND

Matrix-assisted laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOF MS) and the related technique, surface-enhanced laser desorption/ionization (SELDI)-TOF MS, are being applied widely to analyze serum or plasma specimens for potential disease markers.

METHODS

Reports on the basic principles and applications of MALDI-TOF MS were reviewed and related to information on abundance and masses of major plasma proteins.

OUTCOMES

MALDI-TOF MS is a particle-counting method that responds to molar abundance, and ranking of plasma proteins by molar abundance increases the rank of small proteins relative to traditional ranking by mass abundance. Detectors for MALDI-TOF MS augment the bias for detecting smaller components by yielding stronger signals for an equivalent number of small vs large ions. Consequently, MALDI-TOF MS is a powerful tool for surveying small proteins and peptides comprising the peptidome or fragmentome, opening this new realm for analysis. It is complementary to techniques such as electrophoresis and HPLC, which have a bias for detecting larger molecules. Virtually all of the potential markers identified by MALDI-TOF MS to date represent forms of the most abundant plasma proteins.

CONCLUSIONS

Analyses of serum or plasma by MALDI-TOF MS provide new information mainly about small proteins and peptides with high molar abundance. The spectrum of observed proteins and peptides suggests value for applications such as assessment of cardiovascular risk, nutritional status, liver injury, kidney failure, and systemic immune responses rather than early detection of cancer. Extending analysis by MALDI-TOF MS to lower abundance components, such as markers for early-stage cancers, probably will require more extensive specimen fractionation before analysis.

摘要

背景

基质辅助激光解吸/电离飞行时间质谱(MALDI-TOF MS)及相关技术表面增强激光解吸/电离(SELDI)-TOF MS正被广泛应用于分析血清或血浆样本以寻找潜在疾病标志物。

方法

回顾了关于MALDI-TOF MS基本原理和应用的报告,并与主要血浆蛋白的丰度和质量信息相关联。

结果

MALDI-TOF MS是一种对摩尔丰度有响应的粒子计数方法,按摩尔丰度对血浆蛋白进行排序会使小分子蛋白相对于按质量丰度的传统排序的排名提高。MALDI-TOF MS的检测器通过对等量的小离子和大离子产生更强的信号,增加了检测较小成分的偏差。因此,MALDI-TOF MS是一种用于检测构成肽组或片段组的小蛋白和肽的强大工具,为这一新的分析领域开辟了道路。它与诸如电泳和高效液相色谱等对检测大分子有偏差的技术互为补充。迄今为止,几乎所有通过MALDI-TOF MS鉴定出的潜在标志物都是最丰富的血浆蛋白的形式。

结论

通过MALDI-TOF MS分析血清或血浆主要提供了关于具有高摩尔丰度的小蛋白和肽的新信息。观察到的蛋白质和肽的谱图表明其在评估心血管风险、营养状况、肝损伤、肾衰竭和全身免疫反应等应用中具有价值,而非用于癌症的早期检测。将MALDI-TOF MS分析扩展到低丰度成分,如早期癌症标志物,可能需要在分析前进行更广泛的样本分级分离。

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