GATACA

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Data

Data - ToppGene Sources

The vast majority of all data in Gataca is from ToppGene so its credits cover data sources that are used within Gataca. The primary reason for utilizing the same sources between these applications is to help ensure consistancy between them. ToppGene, and Gataca, uses data from over 20 sources.

For ToppGene Credits, please visit:

ToppGene Links (Credits)

Data - GUDMAP

GUDMAP

The GUDMAP data within Gataca is only availble within the GUDMAP interface:

Gataca's GUDMAP

Data - UMLSKS

UMLSKS website

Software

Software - Solr

Solr website

Software - PrototypeJS

Prototype JS website

Prototype JavaScript framework, version 1.7
(c) 2005-2010 Sam Stephenson
 
Prototype is freely distributable under the terms of an MIT-style license.
For details, see the Prototype web site: http://www.prototypejs.org/

Software - script.aculo.us

Script.aculo.us website

NOTE: Only the effects.js and dragdrop.js modules from Script.aculo.us are being used.

// script.aculo.us scriptaculous.js v1.9.0, Thu Dec 23 16:54:48 -0500 2010

// Copyright (c) 2005-2010 Thomas Fuchs (http://script.aculo.us, http://mir.aculo.us)
//
// Permission is hereby granted, free of charge, to any person obtaining
// a copy of this software and associated documentation files (the
// "Software"), to deal in the Software without restriction, including
// without limitation the rights to use, copy, modify, merge, publish,
// distribute, sublicense, and/or sell copies of the Software, and to
// permit persons to whom the Software is furnished to do so, subject to
// the following conditions:
//
// The above copyright notice and this permission notice shall be
// included in all copies or substantial portions of the Software.
//
// THE SOFTWARE IS PROVIDED "AS IS", WITHOUT WARRANTY OF ANY KIND,
// EXPRESS OR IMPLIED, INCLUDING BUT NOT LIMITED TO THE WARRANTIES OF
// MERCHANTABILITY, FITNESS FOR A PARTICULAR PURPOSE AND
// NONINFRINGEMENT. IN NO EVENT SHALL THE AUTHORS OR COPYRIGHT HOLDERS BE
// LIABLE FOR ANY CLAIM, DAMAGES OR OTHER LIABILITY, WHETHER IN AN ACTION
// OF CONTRACT, TORT OR OTHERWISE, ARISING FROM, OUT OF OR IN CONNECTION
// WITH THE SOFTWARE OR THE USE OR OTHER DEALINGS IN THE SOFTWARE.
//
// For details, see the script.aculo.us web site: http://script.aculo.us/

Software - canvasXpress

canvasXpress website

CanvasXpress is a javascript library based on the <canvas> tag implemented in HTML5.

This package is currently being used for the Venn Diagram within SetBuilder. Plans are to utilize it in other areas in the generation of other graphs.

Software - Oracle Enterprise Edition

Oracle website

The data within Gataca is being stored in an Oracle 11g database.

Software - Modernizr

modernizr

modernizr provides simple interfacing to check to see what features are available within the client's browser. This is predomantly used to test for HTML 5 features such as canvas or local storage support.

Software - JQTouch

JQTouch website

JQTouch is being used for the mobile edition of Gataca.

Software - jQuery

JQuery website

jQuery is used within JQTouch only.

Software - tablesort

tablesort website

Copyright (c) 2006 Andrew Tetlaw 
http://tetlaw.id.au/view/blog/table-sorting-with-prototype/

Permission is hereby granted, free of charge, to any person
obtaining a copy of this software and associated documentation
files (the "Software"), to deal in the Software without
restriction, including without limitation the rights to use, copy,
modify, merge, publish, distribute, sublicense, and/or sell copies
of the Software, and to permit persons to whom the Software is
furnished to do so, subject to the following conditions:

The above copyright notice and this permission notice shall be
included in all copies or substantial portions of the Software.

Software - Firebug Light

Firebug Light website

firebugx.js - There is no disclaimer in the original file, but it is an open source project. The main website is http://www.getfirebug.com It is an open source project hosted by Google code.

Link-It Detail - Disease - macular degeneration

Debug Stats

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Reload Stats

Disease (1)

macular degeneration C1720443

Genes (34)

Species:

human : 34

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Species	Gene	GeneId	Gene Name	Evidence
Human	HMCN1	83872	hemicentin 1	GAD, Score=1000, Pubmed Id: 15467524, UMLKSK CUI: C1720443 Title:a novel diagnostic test detects a low frequency of the hemicentin Gln5345Arg variant among northern irish age related macular degeneration patients\|Association:Not Found\|Conclusion:We describe a rapid assay for the genotyping of the Gln5345Arg mutation using real-time fluorescence PCR to facilitate rapid processing of samples through combined amplification and detection steps. These characteristics are suitable for a clinical setting where high throughput diagnostic procedures are required. The frequency of this mutation within the Northern Ireland population has been estimated at 0.2%, concurring with previous findings that this mutation is a rare variant associated with AMD. A rapid diagnostic assay will facilitate a reliable and convenient evaluation of the frequency of the Gln5345Arg mutation and its association with AMD within other populations. GENERIF, Score=901, Pubmed Id: 16885922, UMLKSK CUI: C1720443 None of our subjects (258 macular degeneration,AMD, cases, 72 non-AMD controls) had the Gln5345Arg variant in the HMCN1 gene
Human	PLEKHA1	59338	pleckstrin homology domain containing, family A (phosphoinositide binding specific) member 1	GAD, Score=1000, Pubmed Id: 16174643, UMLKSK CUI: C1720443 Title:\|Association:Not Found\|Conclusion:Not Found
Human	FSCN2	25794	fascin homolog 2, actin-bundling protein, retinal (Strongylocentrotus purpuratus)	GAD, Score=833, Pubmed Id: 14609921, UMLKSK CUI: C1720443 Title:Autosomal dominant macular degeneration associated with 208delG mutation in the FSCN2 gene.\|Association:Y\|Conclusion:The 208delG mutation in the FSCN2 gene produces not only autosomal dominant retinitis pigmentosa but also ADMD in the Japanese population. This mutation is relatively common in Japanese patients with autosomal dominant retinal degeneration and showed clinical variability. CLINICAL RELEVANCE: Autosomal dominant retinitis pigmentosa and ADMD can be caused by the same 208delG mutation. We suggest that mutations in the FSCN2 gene can lead to a spectrum of phenotypes. GENERIF, Score=861, Pubmed Id: 14609921, UMLKSK CUI: C1720443 The 208delG mutation in the FSCN2 gene produces not only autosomal dominant retinitis pigmentosa but also ADMD (autosomal dominant macular degeneration)
Human	FBLN5	10516	fibulin 5	GAD, Score=1000, Pubmed Id: 15269314, UMLKSK CUI: C1720443 Title:Missense variations in the fibulin 5 gene and age-related macular degeneration.\|Association:Not Found\|Conclusion:Missense mutations in the fibulin 5 gene were found in 1.7 percent of patients with AMD. Many variations in other fibulin genes were also found in these patients, and the evolutionary conservation of the affected residues suggests that several of these variations may also be involved in AMD.
Human	PROM1	8842	prominin 1	GENERIF, Score=1000, Pubmed Id: 18654668, UMLKSK CUI: C1720443 Mutant PROM1 found in patients with macular degeneration disrupts photoreceptor disk morphogenesis in mice
Human	BEST1	7439	bestrophin 1	GENERIF, Score=901, Pubmed Id: 16707793, UMLKSK CUI: C1720443 Understanding the structure of the anion conduction pathway of bestrophins provides insights into how mutations produce channel dysfunction and may provide important information for development of therapeutic strategies for treating macular degeneration
Human	VEGFA	7422	vascular endothelial growth factor A	GAD, Score=1000, Pubmed Id: 16384981, UMLKSK CUI: C1720443 Title:Functional Candidate Genes in Age-Related Macular Degeneration: Significant Association with VEGF,VLDLR, and LRP6\|Association:Not Found\|Conclusion:These data suggest that LRP6, VEGF, and VLDLR may play a role in the risk of developing AMD.
Human	TLR4	7099	toll-like receptor 4	GAD, Score=1000, Pubmed Id: 15829498, UMLKSK CUI: C1720443 Title:Toll-like receptor 4 variant D299G is associated with susceptibility to age-related macular degeneration.\|Association:Not Found\|Conclusion:The APOE4 is a risk factor and demonstrated a dose-dependent effect while APOE2 allele conferred a protection to AD. The MTHFR mutation had no correlation with AD.
Human	TLR3	7098	toll-like receptor 3	GENERIF, Score=1000, Pubmed Id: 18753640, UMLKSK CUI: C1720443 The TLR3 412Phe variant confers protection against geographic atrophy in macular degeneration
Human	ELOVL4	6785	ELOVL fatty acid elongase 4	GENERIF, Score=1000, Pubmed Id: 15028284, UMLKSK CUI: C1720443 mutations in ELOVL4 result in the intracellular misrouting of the protein in macular degeneration
Human	SOD2	6648	superoxide dismutase 2, mitochondrial	GAD, Score=1000, Pubmed Id: 11124296, UMLKSK CUI: C1720443 Title:Genetic association of manganese superoxide dismutase with exudative age-related macular degeneration\|Association:Not Found\|Conclusion:The results suggest that manganese superoxide dismutase gene polymorphism is associated with exudative age-related macular degeneration. Microsomal epoxide hydrolase is another enzyme that may be associated with the disease. The exudative form of age-related macular degeneration may have genetic risk factors against oxidative stress and/or effects of xenobiotics. Further association studies in other polymorphic genes for xenobiotic-metabolizing enzymes are needed to elucidate the environmental-genetic interaction in the underlying cause of age-related macular degeneration. GAD, Score=1000, Pubmed Id: 15774926, UMLKSK CUI: C1720443 Title:Association study of detoxification genes in age related macular degeneration\|Association:Not Found\|Conclusion:This study has identified a number of genes requiring further investigation including EPHX1, ADPRT1, CYP2D6, and AhR.
Human	PRPH2	5961	peripherin 2 (retinal degeneration, slow)	GENERIF, Score=861, Pubmed Id: 12902384, UMLKSK CUI: C1720443 Peptide mass-signature genotyping applied to the RDS/peripherin gene of 16 individuals from a family exhibiting autosomal dominant macular degeneration revealed an A-->T transversion in the 5' splice site of intron 2 that is the likely cause of disease
Human	PON1	5444	paraoxonase 1	GAD, Score=1000, Pubmed Id: 15488805, UMLKSK CUI: C1720443 Title:Association of the M55L and Q192R paraoxonase gene polymorphisms with age-related macular degeneration.\|Association:Y\|Conclusion:The M55L and Q192R SNPs of the PON1 gene do not appear to be associated with late AMD in individuals of Anglo-Celtic descent. GAD, Score=1000, Pubmed Id: 15774926, UMLKSK CUI: C1720443 Title:Association study of detoxification genes in age related macular degeneration\|Association:Not Found\|Conclusion:This study has identified a number of genes requiring further investigation including EPHX1, ADPRT1, CYP2D6, and AhR. GAD, Score=1000, Pubmed Id: 11476678, UMLKSK CUI: C1720443 Title:Paraoxonase gene polymorphisms and plasma oxidized low-density lipoprotein level as possible risk factors for exudative age-related macular degeneration\|Association:Y\|Conclusion:These results indicate that the paraoxonase gene polymorphisms may represent a possible genetic risk factor for age-related macular degeneration and that increased plasma oxidized low-density lipoprotein may be involved in the pathogenesis of age-related macular degeneration.
Human	MMP9	4318	matrix metallopeptidase 9 (gelatinase B, 92kDa gelatinase, 92kDa type IV collagenase)	GAD, Score=1000, Pubmed Id: 15834245, UMLKSK CUI: C1720443 Title:MMP-9 microsatellite polymorphism and susceptibility to exudative form of age-related macular degeneration.\|Association:Y\|Conclusion:Longer microsatellites in the promoter of MMP-9 are associated to the exudative form of AMD and to body mass index, a well-known risk factor for the disease.
Human	LRP6	4040	low density lipoprotein receptor-related protein 6	GAD, Score=1000, Pubmed Id: 16384981, UMLKSK CUI: C1720443 Title:Functional Candidate Genes in Age-Related Macular Degeneration: Significant Association with VEGF,VLDLR, and LRP6\|Association:Not Found\|Conclusion:These data suggest that LRP6, VEGF, and VLDLR may play a role in the risk of developing AMD.
Human	HLA-DRB1	3123		GAD, Score=1000, Pubmed Id: 15851575, UMLKSK CUI: C1720443 Title:Association of HLA class I and class II polymorphisms with age-related macular degeneration.\|Association:Not Found\|Conclusion:Significant positive and negative associations exist between HLA alleles and AMD. HLA polymorphisms influence the development of AMD, possibly via modulating choroidal immune function.
Human	HLA-DQB1	3119		GAD, Score=1000, Pubmed Id: 15851575, UMLKSK CUI: C1720443 Title:Association of HLA class I and class II polymorphisms with age-related macular degeneration.\|Association:Not Found\|Conclusion:Significant positive and negative associations exist between HLA alleles and AMD. HLA polymorphisms influence the development of AMD, possibly via modulating choroidal immune function.
Human	CFH	3075	complement factor H	GAD, Score=1000, Pubmed Id: 15870199, UMLKSK CUI: C1720443 Title:A common haplotype in the complement regulatory gene factor H (HF1/CFH) predisposes individuals to age-related macular degeneration\|Association:Not Found\|Conclusion:We propose that genetic variation in a regulator of the alternative complement pathway, when combined with a triggering event, such as infection, underlie a major proportion of AMD in the human population. GAD, Score=1000, Pubmed Id: 16174643, UMLKSK CUI: C1720443 Title:\|Association:Not Found\|Conclusion:Not Found GAD, Score=1000, Pubmed Id: 15761120, UMLKSK CUI: C1720443 Title:Complement factor H variant increases the risk of age-related macular degeneration.\|Association:Not Found\|Conclusion:This common variant likely explains approximately 43% of AMD in older adults. GAD, Score=1000, Pubmed Id: 15761121, UMLKSK CUI: C1720443 Title:Complement factor H polymorphism and age-related macular degeneration.\|Association:Not Found\|Conclusion:Possession of at least one histidine at amino acid 402 increased the risk of AMD 2.7-fold and accounts for 50% of the attributable risk of AMD. GAD, Score=1000, Pubmed Id: 15895326, UMLKSK CUI: C1720443 Title:Strong association of the Y402H variant in complement factor H at 1q32 with susceptibility to age-related macular degeneration.\|Association:Not Found\|Conclusion:A multiplicative model fits the data well, and we estimate the population frequency of the high-risk C allele to be 0.39 (95% confidence interval 0.36-0.42) and the genotype relative risk to be 2.44 (95% confidence interval 2.08-2.83) for TC heterozygotes and 5.93 (95% confidence interval 4.33-8.02) for CC homozygotes. GAD, Score=1000, Pubmed Id: 15761122, UMLKSK CUI: C1720443 Title:Complement factor H polymorphism in age-related macular degeneration.\|Association:Y\|Conclusion:Individuals homozygous for the risk alleles have a 7.4-fold increased likelihood of AMD (95% CI 2.9 to 19). Resequencing revealed a polymorphism in linkage disequilibrium with the risk allele representing a tyrosine-histidine change at amino acid 402. This polymorphism is in a region of CFH that binds heparin and C-reactive protein. The CFH gene is located on chromosome 1 in a region repeatedly linked to AMD in family-based studies. GAD, Score=1000, Pubmed Id: 16379025, UMLKSK CUI: C1720443 Title:Y402H complement factor H polymorphism associated with exudative age-related macular degeneration in the French population\|Association:Y\|Conclusion:These results suggest the contribution of the Y402H polymorphism of the CFH gene to exudative AMD susceptibility also in the French population. This relationship with the CFH may lead to early detection and new strategies for prevention and treatment of AMD.
Human	GPX1	2876	glutathione peroxidase 1	GAD, Score=1000, Pubmed Id: 15774926, UMLKSK CUI: C1720443 Title:Association study of detoxification genes in age related macular degeneration\|Association:Not Found\|Conclusion:This study has identified a number of genes requiring further investigation including EPHX1, ADPRT1, CYP2D6, and AhR.
Human	EFEMP1	2202	EGF containing fibulin-like extracellular matrix protein 1	GENERIF, Score=1000, Pubmed Id: 12242346, UMLKSK CUI: C1720443 EFEMP1 has a role in retinal drusen formation and is involved in the etiology of macular degeneration and Malattia Leventinese GAD, Score=1000, Pubmed Id: 15218514, UMLKSK CUI: C1720443 Title:Analysis of the EFEMP1 gene in individuals and families with early onset drusen.\|Association:Not Found\|Conclusion:The term early onset drusen encompasses a wide range of phenotypes and our findings indicate that it is likely that more than one gene is involved in its causation. It is essential that these clinical phenotypes are well described and categorised to allow greater possibility of success in the search for other disease genes.
Human	EPHX1	2052	epoxide hydrolase 1, microsomal (xenobiotic)	GAD, Score=1000, Pubmed Id: 15774926, UMLKSK CUI: C1720443 Title:Association study of detoxification genes in age related macular degeneration\|Association:Not Found\|Conclusion:This study has identified a number of genes requiring further investigation including EPHX1, ADPRT1, CYP2D6, and AhR.
Human	ACE	1636	angiotensin I converting enzyme	GAD, Score=1000, Pubmed Id: 16384981, UMLKSK CUI: C1720443 Title:Functional Candidate Genes in Age-Related Macular Degeneration: Significant Association with VEGF,VLDLR, and LRP6\|Association:Not Found\|Conclusion:These data suggest that LRP6, VEGF, and VLDLR may play a role in the risk of developing AMD.
Human	CYP2E1	1571	cytochrome P450, family 2, subfamily E, polypeptide 1	GAD, Score=1000, Pubmed Id: 15774926, UMLKSK CUI: C1720443 Title:Association study of detoxification genes in age related macular degeneration\|Association:Not Found\|Conclusion:This study has identified a number of genes requiring further investigation including EPHX1, ADPRT1, CYP2D6, and AhR.
Human	CYP2D6	1565	cytochrome P450, family 2, subfamily D, polypeptide 6	GAD, Score=1000, Pubmed Id: 15774926, UMLKSK CUI: C1720443 Title:Association study of detoxification genes in age related macular degeneration\|Association:Not Found\|Conclusion:This study has identified a number of genes requiring further investigation including EPHX1, ADPRT1, CYP2D6, and AhR.
Human	CYP1A2	1544	cytochrome P450, family 1, subfamily A, polypeptide 2	GAD, Score=1000, Pubmed Id: 15774926, UMLKSK CUI: C1720443 Title:Association study of detoxification genes in age related macular degeneration\|Association:Not Found\|Conclusion:This study has identified a number of genes requiring further investigation including EPHX1, ADPRT1, CYP2D6, and AhR.

XRefs (1)

XRef Types:

cui : 1

ToppGene Datasets:

none : 1

ToppGene Datasets	XRef Type	XRef Id	XRef	Values	Source	Top % Rank
	CUI	C1720443	macular degeneration	0		self

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