Einzeltreffer — DigiBib

Alternative splicing allows a single gene to produce multiple transcript-level splice isoforms from which the translated proteins may show differences in their expression and function. Identifying the major functional or canonical isoform is important for understanding gene and protein functions. Identification and characterization of splice isoforms is a stated goal of the HUPO Human Proteome Project and of neXtProt. Multiple efforts have catalogued splice isoforms as "dominant", "principal", or "major" isoforms based on expression or evolutionary traits. In contrast, we recently proposed highest connected isoforms (HCIs) as a new class of canonical isoforms that have the strongest interactions in a functional network and revealed their significantly higher (differential) transcript-level expression compared to nonhighest connected isoforms (NCIs) regardless of tissues/cell lines in the mouse. HCIs and their expression behavior in the human remain unexplored. Here we identified HCIs for 6157 multi-isoform genes using a human isoform network that we constructed by integrating a large compendium of heterogeneous genomic data. We present examples for pairs of transcript isoforms of ABCC3, RBM34, ERBB2, and ANXA7. We found that functional networks of isoforms of the same gene can show large differences. Interestingly, differential expression between HCIs and NCIs was also observed in the human on an independent set of 940 RNA-seq samples across multiple tissues, including heart, kidney, and liver. Using proteomic data from normal human retina and placenta, we showed that HCIs are a promising indicator of expressed protein isoforms exemplified by NUDFB6 and M6PR. Furthermore, we found that a significant percentage (20%, p = 0.0003) of human and mouse HCIs are homologues, suggesting their conservation between species. Our identified HCIs expand the repertoire of canonical isoforms and are expected to facilitate studying main protein products, understanding gene regulation, and possibly evolution. The network is available through our web server as a rich resource for investigating isoform functional relationships (http://guanlab.ccmb.med.umich.edu/hisonet). All MS/MS data were available at ProteomeXchange Web site (http://www.proteomexchange.org) through their identifiers (retina: PXD001242, placenta: PXD000754).

Titel:	Functional Networks of Highest-Connected Splice Isoforms: From The Chromosome 17 Human Proteome Project.
Autor/in / Beteiligte Person:	Li, HD ; Menon, R ; Govindarajoo, B ; Panwar, B ; Zhang, Y ; Omenn, GS ; Guan, Y
Zeitschrift:	Journal of proteome research, Jg. 14 (2015-09-04), Heft 9, S. 3484-91
Veröffentlichung:	Washington, D.C. : American Chemical Society, c2002-, 2015
Medientyp:	academicJournal
ISSN:	1535-3907 (electronic)
DOI:	10.1021/acs.jproteome.5b00494
Schlagwort:	Animals Humans Mice Protein Isoforms chemistry Proteins chemistry RNA, Messenger genetics Sequence Analysis, RNA Alternative Splicing Chromosomes, Human, Pair 17 Protein Isoforms genetics Proteins genetics Proteome
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article; Research Support, N.I.H., Extramural; Validation Study Language: English [J Proteome Res] 2015 Sep 04; Vol. 14 (9), pp. 3484-91. <i>Date of Electronic Publication: </i>2015 Aug 11. MeSH Terms: Alternative Splicing* ; Chromosomes, Human, Pair 17* ; Proteome* ; Protein Isoforms / genetics ; Proteins / genetics ; Animals ; Humans ; Mice ; Protein Isoforms / chemistry ; Proteins / chemistry ; RNA, Messenger / genetics ; Sequence Analysis, RNA References: Nucleic Acids Res. 2013 Jan;41(Database issue):D110-7. (PMID: 23161672) ; PLoS Comput Biol. 2010 Nov 11;6(11):e1000991. (PMID: 21085640) ; Nucleic Acids Res. 2012 Jan;40(Database issue):D290-301. (PMID: 22127870) ; Bioinformatics. 2014 Dec 1;30(23):3325-33. (PMID: 25115705) ; BMC Genet. 2005 Feb 16;6:8. (PMID: 15715908) ; PLoS Comput Biol. 2012;8(9):e1002694. (PMID: 23028291) ; J Proteome Res. 2011 Dec 2;10(12):5503-11. (PMID: 22003824) ; Proteomics. 2015 Feb;15(4):836-40. (PMID: 25407473) ; Biochem Biophys Res Commun. 2005 Mar 4;328(1):306-11. (PMID: 15670784) ; Dis Markers. 2010;28(4):241-51. (PMID: 20534909) ; J Proteomics. 2014 Apr 4;100:3-7. (PMID: 24145142) ; Trends Genet. 2014 Aug;30(8):340-7. (PMID: 24951248) ; Nat Biotechnol. 2010 Feb;28(2):149-56. (PMID: 20118918) ; Nucleic Acids Res. 2015 Jan;43(Database issue):D222-6. (PMID: 25414356) ; Nat Methods. 2010 Oct;7(10):843-7. (PMID: 20835245) ; Gene. 2006 Oct 1;380(2):63-71. (PMID: 16872759) ; J Proteome Res. 2004 Jan-Feb;3(1):76-83. (PMID: 14998166) ; Cancer Res. 2010 May 1;70(9):3440-9. (PMID: 20388783) ; Database (Oxford). 2015 May 07;2015:bav045. (PMID: 25953081) ; Adv Exp Med Biol. 2007;623:64-84. (PMID: 18380341) ; Nucleic Acids Res. 2004 Jan 1;32(Database issue):D277-80. (PMID: 14681412) ; Nucleic Acids Res. 2012 Jan;40(Database issue):D302-5. (PMID: 22053084) ; Gene. 2005 Jan 3;344:1-20. (PMID: 15656968) ; Nature. 2012 Sep 6;489(7414):101-8. (PMID: 22955620) ; J Comput Biol. 2011 Mar;18(3):305-21. (PMID: 21385036) ; Nucleic Acids Res. 2014 Jan;42(Database issue):D222-30. (PMID: 24288371) ; Nucleic Acids Res. 2011 Jan;39(Database issue):D19-21. (PMID: 21062823) ; J Proteome Res. 2014 Jan 3;13(1):15-20. (PMID: 24364385) ; Comput Syst Bioinformatics Conf. 2006;:341-51. (PMID: 17369653) ; Bioinformatics. 2008 Jan 1;24(1):11-7. (PMID: 18006548) ; PLoS Comput Biol. 2013;9(11):e1003314. (PMID: 24244129) ; J Proteome Res. 2015 Apr 3;14(4):1880-7. (PMID: 25732134) ; J Chem Inf Model. 2013 Mar 25;53(3):717-25. (PMID: 23413988) ; Proteomics. 2014 Dec;14(23-24):2709-18. (PMID: 25265570) ; Cell. 2005 Sep 23;122(6):957-68. (PMID: 16169070) ; J Proteomics. 2013 Sep 2;90:28-37. (PMID: 23603631) ; PLoS One. 2011 Feb 18;6(2):e16880. (PMID: 21365003) ; Nucleic Acids Res. 2013 Jan;41(Database issue):D808-15. (PMID: 23203871) ; PLoS Comput Biol. 2008 Sep 26;4(9):e1000165. (PMID: 18818725) ; J Proteomics. 2014 Jul 31;107:103-12. (PMID: 24802673) ; J Proteome Res. 2014 Jan 3;13(1):173-82. (PMID: 24320163) ; Nat Biotechnol. 2006 Dec;24(12):1565-7. (PMID: 17160063) ; Nat Biotechnol. 2014 May;32(5):462-4. (PMID: 24752080) ; Nat Genet. 2000 May;25(1):25-9. (PMID: 10802651) ; Bioinformatics. 2014 Oct;30(19):2772-8. (PMID: 24919880) ; Proteins. 2001 May 15;43(3):246-55. (PMID: 11288174) Grant Information: U54ES017885 United States ES NIEHS NIH HHS; R21 NS082212 United States NS NINDS NIH HHS; R25 GM086262 United States GM NIGMS NIH HHS; R35 GM133346 United States GM NIGMS NIH HHS; P30 ES017885 United States ES NIEHS NIH HHS; 1R21NS082212-01 United States NS NINDS NIH HHS Contributed Indexing: Keywords: alternative splicing; canonical isoforms; highest connected isoforms; isoform networks Substance Nomenclature: 0 (Protein Isoforms) ; 0 (Proteins) ; 0 (Proteome) ; 0 (RNA, Messenger) Entry Date(s): Date Created: 20150729 Date Completed: 20160606 Latest Revision: 20210513 Update Code: 20231215 PubMed Central ID: PMC4993635

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Functional Networks of Highest-Connected Splice Isoforms: From The Chromosome 17 Human Proteome Project.