RefGenome13Nov07 Phone Conference (Archived): Difference between revisions

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[ACTION ITEM] (all) Please send a fasta file of amino acid sequences, and an explanation of the header lines
[ACTION ITEM] (all) Please send a fasta file of amino acid sequences, and an explanation of the header lines
* Can everyone provide the file?
* Can everyone provide the file?
NOT FINISHED
[ACTION ITEM] (Chris) Provide guidelines and a template for the file they want.





Revision as of 15:34, 13 November 2007

Time: 1 PM CDT, 11 AM PDT, 7 PM BST

Present

  • David Hill (MGI)
  • Pascale (dictyBase)
  • Petra (dictyBase)
  • Rex (dictyBase)
  • Susan (flyBase)
  • Victoria (RGD)
  • Emily (uniProt)
  • Tanya (TAIR)
  • Donghui (TAIR)
  • Stacia (SGD)
  • Mary (MGI)
  • Rachel (UniProt)
  • Simon (RGD)
  • Kimberly (wormbase)
  • Ranjana (wormbase)
  • Chris Mungall
  • Amelia Ireland

Rotation System for selecting genes

  • Comments from Tanya and Donghui:

- It was hard to pick human/E coli but Pascale improved the list - People liked the list

Web presence

Amelia (web page), Susan, Rex, Petra (content)

- Emily: might be a good idea to make those annotations available - Rex: yes, I'm sure people would like to download all this data as a single set - [ACTION IETM] all: Plan: everyone will look at the draft and Amelia will put it up in ~ 1 week

Orthology determination

1) Kara started to collect sequences from all groups. Questions:

  • At the meeting at Princeton, the plan was for each MOD participating in the Ref. Genome project to provide a protein set, in fasta format. Then, as a start, here at Princeton, we'd do an all vs. all BLAST, so that the same BLAST results can be given to the groups developing ortholog identification methods (eg InParanoid, OrthoMCL, etc) with the idea that the results of the methods can then be more easily compared/assessed if the same input sequences and BLAST results were used. It'll probably take 3-4 weeks for the computation to be done on our current system

[ACTION ITEM] (all) Please send a fasta file of amino acid sequences, and an explanation of the header lines

  • Can everyone provide the file?

NOT FINISHED [ACTION ITEM] (Chris) Provide guidelines and a template for the file they want.


2) OMA browser Doug, Pascale While talking with Amos Bairoch at the biocuration meeting, Amos informed us of another orthology prediction option that at least I have not heard mentioned before. OMA browser

This recent pub describes the resource: A Schneider, C Dessimoz and GH Gonnet (2007)

Pros:

  • Already includes all the ref. genome species, and a total of 421 species in the most recent release (June '07).
  • Is being maintained and updated, next release in Nov. '07
  • I have communicated with Christophe Dessimoz to inquire about the use of more recent D.rerio sequences in the next release of OMA and he seemed amiable and willing to field comments and suggestions

Cons:

  • At the moment it works primarily with Ensembl gene IDs, Ensembl protein IDs and genbank protein IDs

Perhaps if we each produced a protein file of our choosing, including MOD gene IDs, he would be able to include that in the next release of OMA? He might even be willing to work on interface improvements that would help us out if we ask nicely.

Thought the group might want to look at this resource so we can discuss it at the next Ref. Genome conf. call.

For your reference, I included some raw data for the OMA group corresponding to the Human ACHE gene. ACHE has been included in the Ref. Genome set for a long time. The Ref Genome tables suggest that there are orthologs found in Mouse, Rat, Worm, Fly and zebrafish. The OMA group below only seems to include Human, mouse, zebrafish, and dicty. I didn't check if the OMA-identified ortholog corresponds to the Ref. Genome specified orthologs or look further into the discrepancies.

### OMA group 13441 ###
 BRARE14851    ENSDARG00000031796; CAC19790.1    ENSDARP00000052988
 HUMAN11630    ENSG00000087085; AAH26315.1; AAH36813.1; AAH94752.1    ENSP00000350037
 MOUSE21200    ENSMUSG00000023328; AAA53521.1; AAH46327.1; AAK28816.1; BAC31228.1; BAC31641.1; BAC32595.1; BAE24373.1; CAA39867.1    ENSMUSP00000024099
 XENTR14267    ENSXETG00000017226    ENSXETP00000037518
 CANFA05639    ENSCAFG00000014054    ENSCAFP00000020717
 CIOIN01178    ENSCING00000004635    ENSCINP00000009596
 FUGRU18051    SINFRUG00000120974    SINFRUP00000127687
 BOVIN17961    ENSBTAG00000001139; AAC64270.1; AAI23899.1    ENSBTAP00000001512
 PANTR09106    ENSPTRG00000019514    ENSPTRP00000033412
 DICDI06813    DICDI_4.1323    XP_638122.1
 MONDO08985    ENSMODG00000004882    ENSMODP00000006010
 MACMU04752    ENSMMUG00000021257    ENSMMUP00000027995
 LOXAF09401    ENSLAFG00000007735    ENSLAFP00000006495
 DASNO05327    ENSDNOG00000003865    ENSDNOP00000002974
 GASAC21097    ENSGACG00000000728    ENSGACP00000000940
 OTOGA01101    ENSOGAG00000017244    ENSOGAP00000015447
 TUPGB03889    ENSTBEG00000006472    ENSTBEP00000005591 

Quality control: outlying ISS annotations

Doug, Chris

Doug raised an important point on the email list: I was wondering what people think of Ref. Genome annotations by ISS that seem to be off by themselves in a graph? I see these quite often in Mary's graphs, and I always wonder how they got there. Possibilities include: 1: ISS annotations where the thing that was ISS'ed to is now gone (bad bad bad) 2: ISS to genes from a non-ref genome species 3. ISS to genes which would not be considered orthologous to the gene being annotating

Just wondering what others think of these and how we can find cases of #1, which specifically need to be updated.

Quality control: Misused terms

Pascale, David, all

Annotation of variants

We need to consider the potential impact of annotating to different forms of the gene (alternatively spliced, processed, etc). For now we will document how each database deals with those: [ACTION ITEM]: (all): provide the method you use for capturing the exact gene product being annotated on this page: Variant_annotation


Review Action items

[ACTION ITEM] (Jim): Provide the set of conserved genes found by InParanoid that are conserved in all 12 species (660 or so); we might want to prioritize this list by ascending order of number of annotations to target unannotated genes (who can do that?) [DONE] 'Suggestions' spreadsheet (look for the "conserved Hs-Ec" sheet) Pascale also marked which genes we've already curated. Prioritization is not yet done

[ACTION ITEM] (GOA): Convert the ensembl IDs from the human-E. coli list to UniProt IDs [DONE] (Pascale) I converted to entrez and HGNC. The UniProt ID was not easy to work with since there was often more than one ID. The table now has human gene names and the two IDs.

[ACTION ITEM] (Val): Provide the list of 207 genes conserved between pombe and human with no annotation/information [DONE but] pombe gene IDs were sent; we need to add them to the 'to do' spreadsheet in the same format

[ACTION ITEM] (Ruth): send the HGNC list of genes with few annotations (potential 'bleeding edge' genes) [ON HOLD] until Varsha is back

[ACTION ITEM]: Emily, David: provide guidelines to submit those annotations to GOA Other taxa annotations. [DONE] see Other_taxa_annotations; also Pascale added a link to this page from our Ref Genome main page under 'Annotation'

[ACTION ITEM] Amelia (web page), Susan, Rex, Petra (content), work on web presence : Report by next meeting

[ACTION ITEM]: David will produce some examples of the function-process links.

Not done, but Suzi and Amelia are going to try to mine these from Reactome instead. It would still be interesting to have this information as it should help annotation consistency. Documentation is available Function-Process_Links

[ACTION ITEM]: For orthology determination: Suzi and Karen E will generate a page where all sequences will be available [DONE???] GFF3 for most databases Reference_Genome_sequence_annotation Question: should we add a link to FASTA files there as well?

[ACTION ITEM]: (Judy) contact/meet with people who have made tools for orthology determination on behalf of the GOC to see if they can help us (that possibly includes re-running the analyses using the most recent set of sequences and proper IDs)

  • Compara, Homologene, TreeFam, in paranoid, others?

[ACTION ITEM]: Kara, Stacia: run the P-POD over the full ref genomes set? analysis on the ref genome data set. Need computational pipeline with existing resources. Currently takes 3 weeks to do 8 species all v all. Goal was set for February 2008 to include all ref genome sets.

[ACTION ITEM]: (developers/software group): consider the potential impact of annotating to different forms of the gene (alternatively spliced, processed, etc). For now we will document how each database deals with those:

[ACTION ITEM]: (all): provide the method you use for capturing the exact gene product being annotated on this page: Variant_annotation

[ACTION ITEM] (Chris, Mike, Rex): Provide Ref genome reports on a regular basis

[ACTION ITEM] (Donghui): Check which IDs TAIR needs to provide for the reports. [We need to provide the TAIR gene accession ids in the spreadsheet instead of the AGI identifiers. -Tanya]

[ACTION ITEM] (Pascale, Doug, ): Provide guidelines for filling the google spreadsheet (IDs, where to put notes, how many ortholog per row (1), etc) [STARTED] Procedure_for_filling_Genome-Specific_spreadsheets

[ACTION ITEM]: (Chris) generate reports for potential misannotations (ND annotations for completed genes, etc). [DONE] Reference_Genome_Database_Reports We can request different reports. What do we do now?

[ACTION ITEM]: (Pascale) generate list of terms that often have incorrect annotations to check for consistent use of the term

In progress, Misused_terms

[ACTION ITEM] (Tanya Berardini, Emily Dimmer, Pascale Gaudet, David Hill, Chris Mungall, Kimberly Van Auken): Write up recommendations for usage of ISS, IEA, IC: Report by next meeting???


[ACTION ITEM] (Judy Blake) Contact NCBI/NLM/OMIM to link to reference genome genes

New Action items

[ACTION IETM] all: Plan: everyone will look at the draft and Amelia will put it up in ~ 1 week