This directory contains data for the IPD-IMGT/HLA database. The IPD-IMGT/HLA database is a specialist sequence database for sequences of the human histocompatibility complex. This directory contains the IPD-IMGT/HLA flat files and documentation.
As of Release 3.56.0, due April 2024, all large files (>100MB) will be provided as compressed files rather than utilise Git LFS, which was previously required. This currently includes the hla.dat, xml/hla.xml, xml/hla_ambigs.xml and hlagen.fasta. This has been done to simplify the cloning process and also due to escalating and unpredictable costs in providing the files using Git LFS from a public repository. All compressed files will use the [ZIP format](https://en.wikipedia.org/wiki/ZIP(file_format)). This formatting change will be applied to all branches.
Previously the repository has required the use of the Git LFS tools (https://git-lfs.github.com) to handle files over 100MB in size. Whilst all hla.dat files are now provided as a zipped file, any pulls from previous commits for Release 3.55.0 and earlier will still require Git LFS. Please use this when cloning the repository to ensure the larger files are downloaded correctly. If Git LFS is not used then large files will contain pointers to the Git LFS location rather than the data required.
The directory also contains the HLA sequences in a number of formats. Within the following folders, the various format types are explained briefly here:
Files designated “X_prot.txt”, where X is a locus or gene, contain protein sequences. Please note that alleles that contain non-coding variations may be identical at the protein level.
Files designated “X_nuc.txt”, where X is a locus or gene, contain the nucleotide coding sequences (CDS). Please note that alleles that contain non-coding variations may be identical at the CDS level.
Files designated “X_gen.txt”, where X is a locus or gene, contain genomic DNA sequences. Please note that for alleles that do not possess genomic sequences there will be no entry in the file, or where there is only a single genomic sequence at the locus, a file will not be produced.
For further information on the construction of these text files, please refer to the description available here: https://www.ebi.ac.uk/ipd/imgt/hla/alignment/help/. To provide consistency in both formatting and to record versioning information, as of version 3.32.0, the header is designated by hash tags at the start of the line.
A zip compressed archive of all the text-format alignment files is available from the top-level directory.
All files in this folder are provided in the FASTA sequence format. Please note the FASTA format contains no alignment information. Due to large file sizes (>100MB) some fasta files will be provided as compressed files. This currently includes the hla_gen.fasta.
Files designated “X_prot.fasta”, where X is a locus or gene, contain protein sequences. Please note that alleles that contain non-coding variations may be identical at the protein level.
Files designated “X_nuc.fasta”, where X is a locus or gene, contain the nucleotide coding sequences (CDS). Please note that alleles that contain non-coding variations may be identical at the CDS level.
Files designated “X_gen.fasta”, where X is a locus or gene, contain genomic DNA sequences. Please note for alleles that do not possess genomic sequences, there will be no entry in the file.
All files in this folder are provided in the MSF sequence format.
Files designated “X_prot.msf”, where X is a locus or gene, contain protein sequences. Please note that alleles that contain non-coding variations may be identical at the protein level.
Files designated “X_nuc.msf”, where X is a locus or gene, contain the nucleotide coding sequences (CDS). Please note that alleles that contain non-coding variations may be identical at the CDS level.
Files designated “X_gen.msf”, where X is a locus or gene, contain genomic DNA sequences. Please note for alleles that do not possess genomic sequences, there will be no entry in the file.
Further information on the OID files can be found in the dedicated README file in the oid directory. As of version 3.32.0, all list files have been converted to csv format, and contain a header. The header is donated by hash tags at the start of the line.
https://github.com/ANHIG/IMGTHLA/blob/Latest/oid/README.md
All files in this folder are provided in the PIR sequence format.
Files designated “X_prot.pir”, where X is a locus or gene, contain protein sequences. Please note that alleles that contain non-coding variations may be identical at the protein level.
Files designated “X_nuc.pir”, where X is a locus or gene, contain the nucleotide coding sequences (CDS). Please note that alleles that contain non-coding variations may be identical at the CDS level.
Files designated “X_gen.pir”, where X is a locus or gene, contain genomic DNA sequences. Please note for alleles that do not possess genomic sequences, there will be no entry in the file.
The files in this folder provide a listing of the T-Cell Epitope Group Assignments for DPB1 proteins. The assignments are taken from the algorithms used for the online tools at https://www.ebi.ac.uk/ipd/imgt/hla/matching/. The file formart is as follows;
Alleles which have yet to be assigned a TCE group using either version are left blank.
Further information on the WMDA files can be found in the dedicated README file in the wmda directory. https://github.com/ANHIG/IMGTHLA/blob/Latest/wmda/README.md
Please refer to the relevant XSD file for information regarding the XML files, which can be found here: https://github.com/ANHIG/IMGTHLA/blob/Latest/xml/hla_ambigs.xsd
Please note in release 3.43.0, there are three XML files for the release, hla.xml, hla_ciwd.xml and hla_ambigs.xml. The hla_ciwd.xml file is an updated version of the hla.xml file and includes the addition of new information from the Common, intermediate and well‐documented HLA alleles in world populations: CIWD version 3.0.0 (https://doi.org/10.1111/tan.13811). This is as new elements have been required to incorporate this data, and the CWD version 2.0.0 data has been recoded to the same structure. In release 3.44.0 and onwards, hla_ciwd.xml will replace hla.xml, and the older format archived.
Please note in release 3.53.0, there was a change made to the hla.xml. The releaseversions tag attribute releasestatus has been changed to a binary flag containing either "Public" or "Deleted" to allow for easier filtering of deleted alleles. In addition a releasecomments attribute has been added containing information about changes to this allele with this verison of the database, this contains the information previously stored in the releasestatus attribute.
Please note in release 3.55.0, there are three XML files for the release, hla.xml, hla_new.xml and hla_ambigs.xml. The hla_new.xml is an updated version of the hla.xml and includes a new release tag containing version and date information for the release. In release 3.56.0 and onwards, hla_new.xml will replace hla.xml, and the older format archived.
Lists of alleles for different versions of the database are now included in this single folder due to the large number of files.
These filenames take the format Allelelist.XXXX.txt with the XXXX in the file denotes a particular release. These files are a csv format detailing for each allele the official name used in each release of the database.
The top-level directory contains the following files;
The top-level directory contains the following lists, in order to provide consistency in both formatting and to record versioning information, as of version 3.32.0, all list files have been converted to csv format, and contain a header. The header is designated by hash tags at the start of the line.
The database version number, IPD-IMGT/HLA 3.44.0 2021-04-20 b9d9ef7, can be interpreted as;
The major release number contains three key fields, the first is the nomenclature version, which is currently 3. The second is the quarterly release number, which is incremented by 1 every January, April, July and October with each subsequent release. The final third number represents the sequence version. A '0' is used for the primary quarterly release, and only incremented if any subsequent interim path or update contains a change to a valid base (not a * or a .) in either the nucleotide (both cDNA and gDNA) or protein sequence. Changes to the positioning of indels, or unsequenced bases are not included if the raw sequence remains unchanged.
For information on the IPD-IMGT/HLA Database please see the website at: http://www.ebi.ac.uk/ipd/imgt/hla
Additional information on sequence file formats is available from: http://www.ebi.ac.uk/ipd/imgt/hla/download/
For any other information please contact hla@alleles.org.
We have chosen to apply the Creative Commons Attribution-NoDerivs License to all copyrightable parts of our databases, which includes the sequence alignments. This means that you are free to copy, distribute, display and make commercial use of the databases in all legislations, provided you give us credit by citing the following;
Barker D, Maccari G, Georgiou X, Cooper M, Flicek P, Robinson J, Marsh SGE The IPD-IMGT/HLA Database Nucleic Acids Research(2023), 51(D1): D948-D955
Robinson J, Barker D, Marsh SGE 25 years of the IPD-IMGT/HLA Database. HLA(2024),103(6): e15549
Robinson J, Malik A, Parham P, Bodmer JG, Marsh SGE: IMGT/HLA - a sequence database for the human major histocompatibility complex Tissue Antigens (2000), 55:280-287
We are strongly opposed to the mirroring of the data contained on our sites, both hla.alleles.org and the IPD-IMGT/HLA Database, and would ask that rather than mirror the information, appropriate links are provided where applicable.
If you intend to distribute a modified version of our data, you must ask us for permission first, please contact hla [at] alleles [dot] org for further details of how modified data can be reproduced.
The development of the IPD-IMGT/HLA Database was funded by an EU BIOTECH grant. The work of maintaining and updating the database has been supported in the past by the Imperial Cancer Research Fund, the National Institute of Health, the National Marrow Donor Program (NMDP) and more recently by the Anthony Nolan Trust. The continual maintenace and any further development of the database relies on alternate sources of financial support, which are actively been sought for the continued maintenance of the database. The Sequence.org initiative at the NMDP has solicited funds from institutions and companies who produce HLA typing reagents, typing systems, and instrumentation or that otherwise utilise these databases in critical components of their business. To learn more about how your business can support the IPD-IMGT/HLA Database, please contact: Anna Bedard, (Email: abedard [at] nmdp [dot] org), Be The Match Foundation.
If you intend to use any of the data found on our sites for commercial use, we would ask you to consider funding the database and the work we do. Without continued funding the database cannot be maintained.
Where discrepancies have arisen between reported sequences and those stored in the database, the original authors have been contacted where possible, and necessary amendments to published sequences have been incorporated. Future sequencing may identify errors and the WHO Nomenclature Committee would welcome any evidence that helps to maintain the accuracy of the database. We therefore make no warranties regarding the correctness of the data, and disclaim liability for damages resulting from its use. We cannot provide unrestricted permission regarding the use of the data, as some data may be covered by patents or other rights. Any medical or genetic information is provided for research, educational and informational purposes only. It is not in any way intended to be used as a substitute for professional medical advice, diagnosis, treatment or care.
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