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'''This created a set of 4364 receptor genes (prior to manual curation)''' |
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'''This created a set of 3209 Ligand genes (prior to manual curation)''' === Extracellular Matrix === Although these molecules were not used for the calculation of the resulting interaction network they were still collected and curated. '''Extracellular Matrix (ECM) genes were defined based on''' 1. the GO terms: * GO:0031012 - extracellular matrix * GO:0005578 - proteinacious extracellular matrix * GO:0005201 - extracellular matrix structural constituent * GO:1990430 - extracellular matrix protein binding * GO:0035426 - extracellular matrix cell signalling '''This created a set of 433 ECM genes (prior to manual curation)''' |
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After curation the resulting ligand, receptor and ecm sets consisted of: * Receptors - 1851 genes. * Ligands - 1593 genes. * ECM - 433 genes. In each of the above sets there are genes that were defined to multiple types. |
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== Download Data == 1. [[attachment:ligands.txt|Ligands]] - table of ligands. (contains HGNC symbol as well as classification (Ligand, Ligand/ECM, Ligand/Receptor, Ligand/ECM/Receptor) 1. [[attachment:receptors.txt|Receptors]] - table of receptors. (contains HGNC symbol as well as classification (Receptor, Receptor/ECM, Ligand/Receptor, Ligand/ECM/Receptor) 1. [[attachment:ecm.txt|ECM]] - table of ECM. (contains HGNC symbol as well as classification (ECM, ECM/Receptor, ECM/Ligand, Ligand/ECM/Receptor) 1. [[attachment:protein_types.txt|Protetin types]] - table of unique set of receptor, ligand and ECM genes (contains HGNC symbol as well as classification (Receptor, Ligand, ECM, ECM/Receptor, ECM/Ligand, Receptor/Ligand, Ligand/ECM/Receptor) 1. [[attachment:receptor_ligand_interactions.txt|Ligand - Receptor interaction set]] |
Cell-Cell Interactions
Contents
Overview
Cell-Cell interactions were computed by a similar method as described by Qiao et al (1) . Using a set of proteins designated as receptors, and ligands defined with a set of GO terms (2,3) and other data sources calculate the set of interactions that represent cell-cell interactions (for example Ligand-receptor, receptor-receptor, ...). This analysis is not limited to Cell-Cell interactions. You can define your own protein types, either manually or by choosing different go terms, and create your customized protein-protein interaction network.
Defining Receptor and Ligands
Receptors
Receptor genes were defined based on
- a set of GO terms:
GO:0043235 - receptor complex,
GO:0008305 - integrin complex,
GO:0072657 - protein localized to membrane
GO:0043113 - receptor clustering
GO:0004872 -receptor activity,
GO:0009897 - external side of plasma membrane)
- Uniprot annotations
- search term -"Receptor [KW-0675]" go:0005886 organism:human.
This created a set of 4364 receptor genes (prior to manual curation)
Ligands
Ligand genes were defined based on
- the GO terms:
GO:0005102 - receptor binding
the set of proteins labelled as secreted in the Secretome dataset (http://www.proteinatlas.org/humanproteome/secretome) (4).
This created a set of 3209 Ligand genes (prior to manual curation)
Extracellular Matrix
Although these molecules were not used for the calculation of the resulting interaction network they were still collected and curated. Extracellular Matrix (ECM) genes were defined based on
- the GO terms:
GO:0031012 - extracellular matrix
GO:0005578 - proteinacious extracellular matrix
GO:0005201 - extracellular matrix structural constituent
GO:1990430 - extracellular matrix protein binding
GO:0035426 - extracellular matrix cell signalling
This created a set of 433 ECM genes (prior to manual curation)
Manual Curation
Receptor and ligand lists were further manually curated
- removing genes that were neither receptors or ligands and
- moving misclassified genes were moved to the correct list (i.e. receptors found on the ligand list or vice versa)
After curation the resulting ligand, receptor and ecm sets consisted of:
- Receptors - 1851 genes.
- Ligands - 1593 genes.
- ECM - 433 genes.
In each of the above sets there are genes that were defined to multiple types.
Interaction Data
The set of protien interactions were downloaded from irefindex (version 14) (5). The entire interaction set was filtered to only included interaction that contained receptor-ligand, receptor - receptor, or ligand-ligand interactions where the receptor and ligands were defined by the above process.
Download Data
Ligands - table of ligands. (contains HGNC symbol as well as classification (Ligand, Ligand/ECM, Ligand/Receptor, Ligand/ECM/Receptor)
Receptors - table of receptors. (contains HGNC symbol as well as classification (Receptor, Receptor/ECM, Ligand/Receptor, Ligand/ECM/Receptor)
ECM - table of ECM. (contains HGNC symbol as well as classification (ECM, ECM/Receptor, ECM/Ligand, Ligand/ECM/Receptor)
Protetin types - table of unique set of receptor, ligand and ECM genes (contains HGNC symbol as well as classification (Receptor, Ligand, ECM, ECM/Receptor, ECM/Ligand, Receptor/Ligand, Ligand/ECM/Receptor)
References
Qiao W, Wang W, Laurenti E, Turinsky AL, Wodak SJ, Bader GD, Dick JE, Zandstra PW Intercellular network structure and regulatory motifs in the human hematopoietic system
PubmedAshburner M, Ball CA, Blake JA, Botstein D, Butler H, Cherry JM, Davis AP, Dolinski K, Dwight SS, Eppig JT, Harris MA, Hill DP, Issel-Tarver L, Kasarskis A, Lewis S, Matese JC, Richardson JE, Ringwald M, Rubin GM, Sherlock G. Gene ontology: tool for the unification of biology. The Gene Ontology Consortium. Nat Genet. 2000 May;25(1):25-9
PubmedThe Gene Ontology Consortium. Expansion of the Gene Ontology knowledgebase and resources. Nucleic Acids Res. 2017 Jan 4;45(D1):D331-D338
PubmedUhlén M, Fagerberg L, Hallström BM, Lindskog C, Oksvold P, Mardinoglu A, Sivertsson Å, Kampf C, Sjöstedt E, Asplund A, Olsson I, Edlund K, Lundberg E, Navani S, Szigyarto CA, Odeberg J, Djureinovic D, Takanen JO, Hober S, Alm T, Edqvist PH, Berling H, Tegel H, Mulder J, Rockberg J, Nilsson P, Schwenk JM, Hamsten M, von Feilitzen K, Forsberg M, Persson L, Johansson F, Zwahlen M, von Heijne G, Nielsen J, Pontén F. Proteomics. Tissue-based map of the human proteome. Science. 2015 Jan 23;347(6220)
PubmedRazick S, Magklaras G, Donaldson IM. iRefIndex: a consolidated protein interaction database with provenance. BMC Bioinformatics. 2008 Sep 30;9:405
Pubmed