Analysis of hepatic glycogen‐associated proteins

糖原 蛋白质组学 生物化学 计算生物学 化学 生物 基因
作者
David Stapleton,Chad Nelson,Krishna Parsawar,Donald A. McClain,Ryan Gilbert‐Wilson,Elizabeth Barker,Brant Rudd,Kevin Brown,Wayne Hendrix,Paul O’Donnell,Glendon J. Parker
出处
期刊:Proteomics [Wiley]
卷期号:10 (12): 2320-2329 被引量:82
标识
DOI:10.1002/pmic.200900628
摘要

Abstract Glycogen particles are associated with a population of proteins that mediate its biological functions, including: management of glucose flux into and out of the glycogen particle, maintenance of glycogen structure and regulation of particle size, number, and cellular location. A survey of the glycogen‐associated proteome would be predicted to identify the relative representation of known members of this population, and associations with unexpected proteins that have the potential to mediate other functions of the glycogen particle. We therefore purified glycogen particles from both mouse and rat liver, using different techniques, and analyzed the resulting tryptic peptides by MS. We also specifically eluted glycogen‐binding proteins from the pellet using malto‐oligosaccharides. Comparison of the rat and mouse populations, and analysis of specifically eluted proteins allow some conclusions to be made about the hepatic glycogen sub‐proteome. With the exception of glycogen branching enzyme all glycogen metabolic proteins were detected. Novel associations were identified, including ferritin and starch‐binding domain protein 1, a protein that contains both a transmembrane endoplasmic reticulum signal peptide and a carbohydrate‐binding module. This study therefore provides insight into the organization of the glycogen proteome, identifies other associated proteins and provides a starting point to explore the dynamic nature and cellular distribution of this metabolically important protein population.

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