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. 2016 Mar 23;2(3):185-95.
doi: 10.1016/j.cels.2016.02.015. Epub 2016 Mar 23.

Plasma Proteome Profiling to Assess Human Health and Disease

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Free article

Plasma Proteome Profiling to Assess Human Health and Disease

Philipp E Geyer et al. Cell Syst. .
Free article

Abstract

Proteins in the circulatory system mirror an individual's physiology. In daily clinical practice, protein levels are generally determined using single-protein immunoassays. High-throughput, quantitative analysis using mass-spectrometry-based proteomics of blood, plasma, and serum would be advantageous but is challenging because of the high dynamic range of protein abundances. Here, we introduce a rapid and robust "plasma proteome profiling" pipeline. This single-run shotgun proteomic workflow does not require protein depletion and enables quantitative analysis of hundreds of plasma proteomes from 1 μl single finger pricks with 20 min gradients. The apolipoprotein family, inflammatory markers such as C-reactive protein, gender-related proteins, and >40 FDA-approved biomarkers are reproducibly quantified (CV <20% with label-free quantification). Furthermore, we functionally interpret a 1,000-protein, quantitative plasma proteome obtained by simple peptide pre-fractionation. Plasma proteome profiling delivers an informative portrait of a person's health state, and we envision its large-scale use in biomedicine.

Keywords: apolipoproteins; blood analysis; clinic; disease; human; mass spectrometry; plasma proteome profile.

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  • A Clarion Call for Proteomics.
    Mak HC. Mak HC. Cell Syst. 2016 Mar 23;2(3):135-6. doi: 10.1016/j.cels.2016.03.005. Epub 2016 Mar 23. Cell Syst. 2016. PMID: 27135358 No abstract available.

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