Literature DB >> 35929804

Systematic evaluation of Copper(II)-loaded immobilized metal affinity chromatography for selective enrichment of copper-binding species in human serum and plasma.

Samuel E Janisse1, Vibha A Sharma1, Amanda Caceres1, Valentina Medici2, Marie C Heffern1.   

Abstract

Copper is essential in a host of biological processes, and disruption of its homeostasis is associated with diseases including neurodegeneration and metabolic disorders. Extracellular copper shifts in its speciation between healthy and disease states, and identifying molecular components involved in these perturbations could widen the panel of biomarkers for copper status. While there have been exciting advances in approaches for studying the extracellular proteome with mass spectrometry-based methods, the typical workflows disrupt metal-protein interactions due to the lability of these bonds either during sample preparation or in gas-phase environments. We sought to develop and apply a workflow to enrich for and identify protein populations with copper-binding propensities in extracellular fluids using an immobilized metal affinity chromatography (IMAC) resin. The strategy was optimized using human serum to allow for maximum quantity and diversity of protein enrichment. Protein populations could be differentiated based on protein load on the resin, likely on account of differences in abundance and affinity. The enrichment workflow was applied to plasma samples from patients with Wilson's disease and protein IDs and differential abundancies relative to healthy subjects were compared to those yielded from a traditional proteomic workflow. While the IMAC workflow preserved differential abundance and protein ID information from the traditional workflow, it identified several additional proteins being differentially abundant including those involved in lipid metabolism, immune system, and antioxidant pathways. Our results suggest the potential for this IMAC workflow to identify new proteins as potential biomarkers in copper-associated disease states.
© The Author(s) 2022. Published by Oxford University Press.

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Year:  2022        PMID: 35929804      PMCID: PMC9434637          DOI: 10.1093/mtomcs/mfac059

Source DB:  PubMed          Journal:  Metallomics        ISSN: 1756-5901            Impact factor:   4.636


  56 in total

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Authors:  R Costa; A Gonçalves; M J Saraiva; I Cardoso
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Journal:  J Chromatogr B Analyt Technol Biomed Life Sci       Date:  2013-07-05       Impact factor: 3.205

Review 6.  Recent advances in physiological lipoprotein metabolism.

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Review 7.  The complement system.

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8.  MSFragger: ultrafast and comprehensive peptide identification in mass spectrometry-based proteomics.

Authors:  Andy T Kong; Felipe V Leprevost; Dmitry M Avtonomov; Dattatreya Mellacheruvu; Alexey I Nesvizhskii
Journal:  Nat Methods       Date:  2017-04-10       Impact factor: 28.547

9.  Uncontrolled zinc- and copper-induced oligomerisation of the human complement regulator factor H and its possible implications for function and disease.

Authors:  Ruodan Nan; Jayesh Gor; Imre Lengyel; Stephen J Perkins
Journal:  J Mol Biol       Date:  2008-10-19       Impact factor: 5.469

10.  Transthyretin protects against A-beta peptide toxicity by proteolytic cleavage of the peptide: a mechanism sensitive to the Kunitz protease inhibitor.

Authors:  Rita Costa; Frederico Ferreira-da-Silva; Maria J Saraiva; Isabel Cardoso
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