| Literature DB >> 24214988 |
James Dunbar1, Konrad Krawczyk, Jinwoo Leem, Terry Baker, Angelika Fuchs, Guy Georges, Jiye Shi, Charlotte M Deane.
Abstract
Structural antibody database (SAbDab; http://opig.stats.ox.ac.uk/webapps/sabdab) is an online resource containing all the publicly available antibody structures annotated and presented in a consistent fashion. The data are annotated with several properties including experimental information, gene details, correct heavy and light chain pairings, antigen details and, where available, antibody-antigen binding affinity. The user can select structures, according to these attributes as well as structural properties such as complementarity determining region loop conformation and variable domain orientation. Individual structures, datasets and the complete database can be downloaded.Entities:
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Year: 2013 PMID: 24214988 PMCID: PMC3965125 DOI: 10.1093/nar/gkt1043
Source DB: PubMed Journal: Nucleic Acids Res ISSN: 0305-1048 Impact factor: 16.971
Figure 1.SAbDab’s workflow. Each week new structures from the PDB are analyzed to find antibody chains. These structures are then annotated with a number of properties and stored in SAbDab. Users may access and select this data using a number of different criteria. Structures and annotations can be downloaded individually or as a dataset. Inset, a schematic of the IgG antibody structure and the F fragment formed by the heavy and light variable domains, VH and VL.
SAbDab’s current antibody–antigen complex content
| Antigen type | No. of structures | No. of |
|---|---|---|
| Protein | 604 | 1081 |
| Peptide | 224 | 321 |
| Carbohydrate | 64 | 86 |
| Nucleic-acid | 12 | 15 |
| Hapten | 147 | 224 |
| Total contents | 1624 | 3048 |
Multiple F regions may appear in a single PDB structure.
Figure 2.The number of antibody structures in the PDB is rising rapidly. On an average, six new antibody structures are added to SAbDab each week.
Figure 3.Selected screen-shots of SAbDab (a) The structure summary page for an entry in SAbDab. Detailed information about the structure and a visualization of the antibody and antigen is available. (b) The advanced search form. Structures may be selected using a number of methods. Here, the advanced search selects the required attributes of each structure in the selection. (c) The alignment between a query sequence and a template identified by the template search function. (d) The ABangle orientation search tool. Users may select F structures by choosing specific regions of the VH–VL orientation space.