Literature DB >> 20077415

Investigating protein isoforms via proteomics: a feasibility study.

Paul Blakeley1, Jennifer A Siepen, Craig Lawless, Simon J Hubbard.   

Abstract

Alternative splicing (AS) and processing of pre-messenger RNAs explains the discrepancy between the number of genes and proteome complexity in multicellular eukaryotic organisms. However, relatively few alternative protein isoforms have been experimentally identified, particularly at the protein level. In this study, we assess the ability of proteomics to inform on differently spliced protein isoforms in human and four other model eukaryotes. The number of Ensembl-annotated genes for which proteomic data exists that informs on AS exceeds 33% of the alternately spliced genes in the human and worm genomes. Examining AS in chicken via proteomics for the first time, we find support for over 600 AS genes. However, although peptide identifications support only a small fraction of alternative protein isoforms that are annotated in Ensembl, many more variants are amenable to proteomic identification. There remains a sizeable gap between these existing identifications (10-52% of AS genes) and those that are theoretically feasible (90-99%). We also compare annotations between Swiss-Prot and Ensembl, recommending use of both to maximize coverage of AS. We propose that targeted proteomic experiments using selected reactions and standards are essential to uncover further alternative isoforms and discuss the issues surrounding these strategies.

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Year:  2010        PMID: 20077415      PMCID: PMC3708446          DOI: 10.1002/pmic.200900445

Source DB:  PubMed          Journal:  Proteomics        ISSN: 1615-9853            Impact factor:   3.984


  61 in total

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  15 in total

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8.  Identification of rare alternative splicing events in MS/MS data reveals a significant fraction of alternative translation initiation sites.

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9.  Protein interaction network of alternatively spliced NudCD1 isoforms.

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10.  Impact of Alternative Splicing on the Human Proteome.

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