src/hg/makeDb/trackDb/human/enigma.html 3f6d3b9b6ecc50930f78bc9ce752b0b0950590d5

3f6d3b9b6ecc50930f78bc9ce752b0b0950590d5
lrnassar
  Mon Mar 11 09:58:47 2024 -0700
Adding enigma tracks html page, refs #32914

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+<H2>Description</H2>
+<p>
+
+<div class="warn-note" style="border: 2px solid #9e5900; padding: 5px 20px; background-color: #ffe9cc;">
+<p><span style="font-weight: bold; color: #c70000;">NOTE:</span><br>
+<b>These data are for research purposes only. While the ClinGen data are 
+open to the public, users seeking information about a personal medical or 
+genetic condition are urged to consult with a qualified physician for 
+diagnosis and for answers to personal medical questions.
+</p>
+<p> 
+UCSC presents these data for use by qualified professionals, and even 
+such professionals should use caution in interpreting the significance of 
+information found here. No single data point should be taken at face 
+value and such data should always be used in conjunction with as much 
+corroborating data as possible. No treatment protocols should be 
+developed or patient advice given on the basis of these data without 
+careful consideration of all possible sources of information.
+</p>
+<p> 
+No attempt to identify individual patients should 
+be undertaken. No one is authorized to attempt to identify patients 
+by any means.
+</p> 
+</b>
+</div>
+
+<p>
+The tracks listed here contain data from the ClinGen ENIGMA BRCA1 and BRCA2 
+Expert Panel Specifications to the ACMG/AMP Variant Interpretation 
+Guidelines for BRCA1/BRCA1 Version 1.0.0. The ENIGMA VCEP has adapted 
+the ACMG-AMP codes for the BRCA1 and BRCA2 genes. These include the 
+codes PVS1 (modified PVS1 decision tree), PS3/BS3 (functional data), 
+PP4/BP5 (multifactorial data), PM5_PTC (PTC data, at exon level), 
+the (potentially) clinically important functional domains defined by 
+ENIGMA, and prediction programs (SpliceAI and BayesDel for PP3/BP4).<br><br>
+The data required for the application of these ENIGMA codes are displayed in 5 data tracks:</p>
+<p>
+<ul>
+<li><b>BRCA1/BRCA2 protein domains 1.1.0</b> -
+Shows the (potentially) clinically important functional domains for 
+the genes BRCA1 and BRCA2 as defined by ENIGMA. Data taken from Figure 
+1 of the guidelines document CSpec_BRCA12ACMG-Rules-Specifications_V1.0_23-04-27.
+</li>
+<li><b>BRCA1/BRCA2 exon weights 1.1.0</b> -
+This track shows exon-specific weights for PM5_PTC ACMG code used 
+for application of this code for novel protein termination codon (PTC) 
+variants in an exon where a different proven pathogenic PTC variant 
+has been seen before. Data taken from guidelines document 
+CSpec_BRCA12ACMG_Rules-SupplementaryTables_V1.0_23-04-27.
+</li>
+<li><b>BRCA1/BRCA2 functional assays 1.1.0</b> -
+Summary of BRCA1 and BRCA2 functional assay results reviewed for 
+application of PS3 and BS3 ACMG codes Data taken from guidelines 
+document CSpec_BRCA12ACMG-Rules-Specifications_V1.0_Table-9_23-04-27.
+</li>
+<li><b>BRCA1/BRCA2 splicing 1.1.0</b> -
+Summary of ACMG codes applicable for variants considered against 
+the BRCA1 and BRCA2 PVS1 decision trees. Includes PVS1 and PM5 
+codes recommended for initiation, nonsense/frameshift, deletion, 
+duplication, and splice site (donor/acceptor ±1,2) variants– 
+organized by exon. Data taken from guidelines document 
+CSpec_BRCA12ACMG-Rules-Specifications_V1.0_Table-4_23-04-27.
+</li>
+<li><b>BRCA1/BRCA2 likelihood for PP4 and BP5</b> -
+Summary of BRCA1 and BRCA2 multifactorial likelihood analysis 
+scores (displayed as Combined LR score) for ACMG codes PP4 and BP5. 
+Data taken from Parsons et al. 2019 suppl table HUMU-40-1557-s001_Parson_Multicatorial.xlsx.
+</li>
+</ul>
+</p>
+ 
+<h2>Display Conventions</h2>
+<p>
+<ul>
+<li><b>BRCA1/BRCA2 protein domains 1.1.0</b> -
+Items in <b><font color="red">red</font></b> show clinically relevant 
+protein domains. Mouseover on items shows the name of the domain and the location.
+</li>
+<li><b>BRCA1/BRCA2 exon weights 1.1.0</b> -
+Mouseover on exons (black items) show the transcript, exon number and the PM5_PTC code strength.
+</li>
+<li><b>BRCA1/BRCA2 functional assays 1.1.0</b> -
+Variants assigned with BS3 code in <b><font color="green">green</font></b>, 
+PS3 code in <b><font color="red">red</font></b>, or no code assigned in black. 
+Mouseover on items show variant HGVS nomenclature, assigned ACMG code and code weight.
+</li>
+<li><b>BRCA1/BRCA2 splicing 1.1.0</b> -
+Items show variant positions, <b><font color="red">red</font></b> indicates 
+exon deletions, <b><font color="blue">blue</font></b> exon duplications, purple 
+items indicate variants with supporting RNA-based functional evidence. Mouseover 
+on items show transcript, exon, variant position, possible variant type at 
+that position and assigned ACMG code to the variant.
+</li>
+<li><b>BRCA1/BRCA2 likelihood for PP4 and BP5</b> -
+Variants assigned with PP4 code in <b><font color="red">red</font></b>, BP5 code 
+in <b><font color="green">green</font></b>, and non-informative variants (no code 
+assigned) in grey. Mouseover on items show variant HGVS nomenclature, combined 
+likelihood ratio (LR) score, and assigned ACMG code and strength.
+</li>
+</ul>
+</p>
+
+<h2>Data Access</h2>
+<p>
+The most up-to-date VCEP specifications for application of ACMG/AMP criteria 
+for BRCA1 and BRCA2 genes are freely available at the <a target="_blank" 
+href="https://cspec.genome.network/cspec/ui/svi/affiliation/50087">ClinGen 
+Criteria Specification (CSpec) Registry</a>. This registry is intended to 
+provide access to the Criteria Specifications used and applied by <a 
+target="_blank" href="https://clinicalgenome.org/affiliation/vcep/#ep_table_heading">ClinGen 
+Variant Curation Expert Panels</a> and biocurators in the classification of variants.
+</p>
+
+<h2>Methods</h2>
+<p>
+These data were created and adapted from the files referenced above. Some custom 
+scripting was employed in tasks like mapping variants, adding colors and 
+mouseovers, and producing the desired format. For the complete details on 
+the data processing see the makedoc on our <a target="_blank" 
+href="https://github.com/ucscGenomeBrowser/kent/blob/master/src/hg/makeDb/doc/enigma.txt">github</a>.
+</p>
+
+<h2>Credits</h2>
+<p>
+Thank you to Luis Nassar from the Genome Browser team, Anna Benet-Pagès 
+and Andreas Laner for technical coordination and consultation, and to 
+the ENIGMA consortia for making these data available.</p>
+
+<h2>References</h2>
+
+<p>
+Enigma Guidelines: <a target="_blank" href="https://clinicalgenome.org/affiliation/50087/">https://clinicalgenome.org/affiliation/50087/</a></p>
+<p>
+Enigma Consortium: <a target="_blank" href="https://enigmaconsortium.org/">https://enigmaconsortium.org/</a></p>
+<p>
+Parsons MT, Tudini E, Li H, Hahnen E, Wappenschmidt B, Feliubadal&#243; L, Aalfs CM, Agata S,
+Aittom&#228;ki K, Alducci E <em>et al</em>.
+<a href="https://doi.org/10.1002/humu.23818" target="_blank">
+Large scale multifactorial likelihood quantitative analysis of BRCA1 and BRCA2 variants: An ENIGMA
+resource to support clinical variant classification</a>.
+<em>Hum Mutat</em>. 2019 Sep;40(9):1557-1578.
+PMID: <a href="https://www.ncbi.nlm.nih.gov/pubmed/31131967" target="_blank">31131967</a>; PMC: <a
+href="https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6772163/" target="_blank">PMC6772163</a>
+</p>