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Review

Overcoming the dynamic range problem in mass spectrometry-based shotgun proteomics

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Pages 611-619 | Published online: 09 Jan 2014
 

Abstract

Protein profiling using mass spectrometry technology has emerged as a powerful method for analyzing large-scale protein-expression patterns in cells and tissues. However, a number of challenges are present in proteomics research, one of the greatest being the high degree of protein complexity and huge dynamic range of proteins expressed in the complex biological mixtures, which exceeds six orders of magnitude in cells and ten orders of magnitude in body fluids. Since many important signaling proteins have low expression levels, methods to detect the low-abundance proteins in a complex sample are required. This review will focus on the fundamental fractionation and mass spectrometry techniques currently used for large-scale shotgun proteomics research.

Acknowledgements

This work was supported by the NIH grants RO1 HL67569, PO1 HL 70694 and RR 13186.

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