| Literature DB >> 17430555 |
Pasqualina D'Ursi1, Francesca Marino, Andrea Caprera, Luciano Milanesi, Elena M Faioni, Ermanna Rovida.
Abstract
BACKGROUND: Activated Protein C (ProC) is an anticoagulant plasma serine protease which also plays an important role in controlling inflammation and cell proliferation. Several mutations of the gene are associated with phenotypic functional deficiency of protein C, and with the risk of developing venous thrombosis. Structure prediction and computational analysis of the mutants have proven to be a valuable aid in understanding the molecular aspects of clinical thrombophilia.Entities:
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Year: 2007 PMID: 17430555 PMCID: PMC1885840 DOI: 10.1186/1471-2105-8-S1-S11
Source DB: PubMed Journal: BMC Bioinformatics ISSN: 1471-2105 Impact factor: 3.169
Figure 1The Home Page of the Database. The database menu is on the left-hand side of the web page. It contains links to general information about gene, protein and clinical features of protein C deficiency, a link to the search in the database, links to mutations analysis tools, to authors correspondence, to a submission form for new mutations and to external web resources. Images are examples of structural details.
Figure 2Detailed view of an entry of the database. The example refers to the variant G216D. The user may find general information about the variant, the available references and cross-references. A great importance is given to the structural aspects of the mutation. In the 3D gallery the user can access the PDB coordinates of the modelled mutant and the VRML format for visualization and a link to 3D notes.
Figure 3A 3D-notes page. The example refers to the variant G216D. Information on the physico-chemical properties of the mutant residue compared to wild-type (i.e. charge, hydrophobicity, solvent accessibility) is given, hydrogen bonds and hydrophobic interactions are listed. Additional data resulting from computational studies, such as electrostatic potential calculation, and the predicted effect of mutation are also reported.