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Alexander Wait Zaranek, 02/08/2010 12:54 PM

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 = Genotype + Environment = Trait (GET) Evidence Database = 
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The '''GET Evidence''' project was started by Abraham Rosenbaum, Joe Thakuria, Xiaodi Wu and Alexander Wait Zaranek to help the [http://personalgenomes.org Personal Genome Project], the clinical genetics community, and, the general public interpret individual genomes.  The database is closely integrated with [wiki:Trait-o-matic].
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You can find the PGP production server at:
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 * http://evidence.personalgenomes.org
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A development sandbox can be found at: 
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 * http://evidence-dev.personalgenomes.org
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Many contributors helped make '''GET Evidence''' possible. You can find specific contributions at: 
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 * http://evidence.personalgenomes.org/editors
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Please help the project by editing the database or making suggestions on the wiki!  
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 == Field Descriptions and Editing Guidelines ==
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 === Short Summary === 
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 * free text providing a one line summary of clinical action to be undertaken given this variant (possibly modified by known phenotypes). 
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 === Variant Quality Data === 
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Each of these fields is a sliding scale of 0-5 where 0 represents no evidence and 5 strong evidence that the Impact is correct. Where the data is not entered the default is N/A. When Genetests and/or the literature correlate this variant with a number of phenotypes the impact should be reported for the most extreme condition
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 a. ''In silico'': One star for each consistent prediction and one start subtracted for conflicting results from:
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  i. evolutionary conservation (minimum of three species)
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  i. presence in active domain 
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  i. SIFT 
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  i. !PolyPhen 
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  i. NBLOSUM 
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  i. GVGD
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  i. Other variants in this gene cause similar disease 
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  i. etc... 
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 a. ''In vitro'': One star for each experiment supporting the result, and penalize one star for conflicting results from: 
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  i. enzyme extracts 
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  i. cell lines  
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  i. animal models
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  i. etc... 
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 a. Case/Control: Odds Ratio etc... 
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  i. 0 stars for OR<1
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  i. 1 star for 1<OR<1.5
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  i. 2 stars for 1.5<OR<2
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  i. 3 stars for 2<OR<3 
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  i. 4 stars for 3<OR<5
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  i. 5 stars for OR>5 
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 a. Familial Disease Segregation
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  i. 0 stars for no segregation (LOD < -2)
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  i. 1 star if segregation exists in one family pedigree
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  i. 2 stars for segregation in more than one family with some conflicting information (e.g. asymptomatic carrier of young age or possibility of second causative mutation)
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  i. 3 stars for more than one family no conflicting information
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  i. 4 stars for LOD > 2
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  i. 5 stars for LOD > 3.
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 a. Clinical Outcomes: The quality of studies investigating the effectiveness of action based on the described impact of this mutation given a specific phenotype/family history
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  i. 0 stars for poor outcome for intervention (diagnostic and medical)
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  i. 1 star no proven benefit for intervention
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  i. 2 stars anecdotal evidence for intervention (unpublished results) 
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  i. 3 stars weak evidence for intervention (less than 10 cases)
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  i. 4 stars standard recommendations for further intervention in development (or more than 10 cases)
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  i. 5 stars for further intervention in routine use  
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 === Impact === 
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When Genetests and/or the literature this variant with a number of phenotypes the impact should be reported for the most extreme condition.
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 a. Pathogenic: Causative for disease; the evidence must have four stars in one of the clinical categories and at least three stars in two other categories. 
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 a. Likely Pathogenic:
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 a. Likely Benign
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 a. Benign
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 a. Likely Protective
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 a. Protective: Protective from disease; the evidence must have four stars in one of the clinical categories and at least three stars in two other categories.
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 a. Unknown Clinical Significance 
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 a. Likely Responsive
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 a. Responsive
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 a. Likely Not Responsive
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 a. Not Responsive
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 a. Not yet reviewed 
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 === Inheritance Pattern === 
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 a. Dominant
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 a. Recessive
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 a. Other: A defined form of inheritance that is neither dominant or recessive (e.g. modifier, co-dominant, incomplete penetrance). These variants will get prioritized due to their potential phenotypic affect should the additional factors be present.
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 a. Undefined: Undefined in the literature.
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 a. Unknown: The default value for all variants and all variants without literature.
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 === Summary of published research, and additional commentary === 
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 * Free text providing a comprehensive review of the variant including youngest age of onset, oldest age of onset and oldest asymptomatic individual. 
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 === Allele Frequency === 
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 * Automatically generated frequencies for the !HapMap Project, 1000 Genomes Project and the weighted average of the two.  Sub-population frequencies and homozygous/heterozygous break-downs are currently not shown. 
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 === Publications === 
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 * User-entered publications and user entered synopses of the relevant details from the publication. A short summary is also entered for each paper (as above).
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 === Genomes ===  
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 * Automatically generated list of all genomes from Trait-o-matic in which this variant is seen. Additionally, specific actions taken by each individual harboring the variant can be reported.
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 === Other External References === 
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These are automatically generated by web "robots":  
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   a. dbSNP: The link to the dbSNP entry for this nucleotide position (for this nucleotide change?)
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   a. Genetests: Link to all clinical laboratories performing diagnostic tests on this gene and the list of diseases that the labs are looking for.
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   a. Web Search Results: A web search for this exact variant using the Yahoo search engine
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 === Edit History ===
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 * Automatically generated history of all page edits with the contributor's name.
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 == To Do ==
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 * [wiki:GET-Evidence/23andWe]
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 == Suggestions == 
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 * your suggestion here.