Extensive analysis of the human platelet proteome by two-dimensional gel electrophoresis and mass spectrometry |
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Authors: | García Angel Prabhakar Sripadi Brock Chris J Pearce Andrew C Dwek Raymond A Watson Steve P Hebestreit Holger F Zitzmann Nicole |
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Affiliation: | Oxford Glycobiology Institute, Department of Biochemistry, University of Oxford, South Parks Road, Oxford, UK. angel@glycob.ox.ac.uk |
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Abstract: | Platelets play a key role in the control of bleeding and wound healing, contributing to the formation of vascular plugs. Under pathologic circumstances, they are involved in thrombotic disorders, including heart disease. Since platelets do not have a nucleus, proteomics offers a powerful alternative approach to provide data on protein expression in these cells, helping to address their biology. In this publication we extend the previously reported analysis of the pI 4-5 region of the human platelet proteome to the pI 5-11 region. By using narrow pI range two-dimensional electrophoresis (2-DE) for protein separation followed by high-throughput tandem mass spectrometry (MS/MS) for protein identification, we were able to identify 760 protein features, corresponding to 311 different genes, resulting in the annotation of 54% of the pI 5-11 range 2-DE proteome map. We evaluated the physicochemical properties and functions of the identified platelet proteome. Importantly, the main group of proteins identified is involved in intracellular signalling and regulation of the cytoskeleton. In addition, 11 hypothetical proteins are reported. In conclusion, this study provides a unique inventory of the platelet proteome, contributing to our understanding of platelet function and building the basis for the identification of new drug targets. |
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Keywords: | Electrospray ionisation-tandem mass spectrometry Platelets Two-dimensional gel electrophoresis |
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