To model the faknt p53 peptide interaction, the dock 6. Identification of new inhibitors of mdm2p53 interaction via pharmacophore and structurebased virtual screening. The interaction of p53 and mdm2 genes in cancers, in silico studies and phylogenetic analysis jayaraman a1, jamil k1, raju s2 1school of biotechnology and bioinformatics, jawaharlal nehru. Mechanistically, ectopically expressed sbds triggered by, for example, ribosomal stress binds to the transactivation domain of p53 and perturbs the mdm2 p53 interaction, consequently. Inactivation of p53 is the most prevalent defect in human cancers. Pmc free article laurentpuig p, beroud c, soussi t. We used default parameters in the pharmacophore module in discovery studio. Mutant p53 interactome identifies nardilysin as a p53r273h. Please note that cellline data are also included in the dataset od somatic mutations. The interaction of p53 and mdm2 genes in cancers, in. It includes a rigidbody structural comparison of target proteins to known templates of proteinprotein interfaces and a flexible refinement using a docking energy function.
For hierarchical clustering or to look at trends in the p53 chipseq data using the orio online resource for integrative omics platform. By using an approach similar to that of clinical metaanalyses, we clearly showed that several published studies have a p53 mutant activity profile that differs significantly from the normal distribution observed in other studies and can have a profound effect on the analysis of the p53 mutation database. The p53 mutations in cell lines compendium is a novel and original application that provides an id card for each cell line included in the umd tp53 database. Tp53 mutations, expression and interaction networks in. Software and program schrodingers maestro visualization program and accelrys discovery studio 4. Inhibitors of the mdm2 p53 interaction that restore the functional p53 constitute potential nongenotoxic anticancer agents with a novel mode of action. In contrast, unmodified ctd strengthens p53 interactions with cruciform targets. Dnabinding protects p53 from interactions with cofactors involved in transcriptionindependent functions. This p53 family network displays interplays as it exhibits common. The umd tp53 variant database includes a full description of the 6,870 tp53 variants found in the database. Although the associations of p53 dysfunction, p53 interaction networks, and oncogenesis have been widely explored 5, a systematic analysis of tp53 mutations and the related interaction networks in various types of human cancers is lacking.
This site still includes former features, such as tp53 history, tp53 information or the tp53 mutation database. The tumour suppressor p53 is a transcription factor that binds dna in the vicinity of the genes it controls. See detailed information on database contents in the users guide. The tumor suppressor protein p53 plays an important role in preventing tumor. The rcsb pdb also provides a variety of tools and resources. Modifications or deletion of the regulatory sequence in the ctd is required for p53 binding to target sites in bform dna. The umd tp53 variant database includes a full description of the 6,870 tp53 variants found in the database with 70 novel features associated with each tp53 variant. Database and software for the analysis of mutations in the. Database protein sequence the protein sequences of p53 gene are showed in below table. Data tables and visualizations are interactive enabling scientists to look for novel patterns in the data.
We employed prism 64,65 to screen 54 different potential interaction partners for the p53 dbd. B p53, p63 and p73 interaction networks from interologous interaction database visualised with navigattor 2. Higher parp1 protein levels and par proteins were detected in mtp53 r273h than in wildtype p53. Algorithm for prediction of tumour suppressor p53 affinity. The nci database was further filtered with above models. Prism is a motifbased software to predict proteinprotein interactions. A p53 mutation database has been createdsee beroud et al. Our current index contains 1,783,645 raw protein and genetic interactions from major model. The structure viewer allows the user to view existing human p53.
The structures indicate how the substituents of a small molecule that bind to the three subpockets of the mdm2x p53 interaction. Explaining oscillations and variability in the p53mdm2. Be aware that many cell lines may have different tp53 status according to different studies. It is well known that stress induces an increase in levels of p53 which in turn leads to an increase in the transcription of mdm2.
In recent years, there has been an exponential increase in the number of p53 mutations identified in human cancers. Qsar models for isoindolinonebased p53 mdm2 interaction inhibitors using linear and nonlinear statistical methods xiaowu dong1, jingying yan1, dong lu1, peng wu1, jiadi gao1, tao liu1, bo. See how interaction crm software can optimize your firms marketing and business development strategy. This site still includes former features, such as tp53 history, tp53 information or the tp53 mutation database, but these features have been updated to take into account the most recent developments in this exciting field. Mlr and svmr models were further applied to evaluate its ability in picking up active molecules p53mdm2 interaction inhibitors from an in.
One pathway for stabilization of p53 is via the kinase atm, which is activated by dna damage and phosphorylates p53 close to its mdm2 binding site, so blocking its interaction. Biogrid is an online interaction respository with data compiled through comprehensive curation efforts. Cartello,2 lisa cui, christophe beroud, and thierry soussi. Biogrid database of protein, chemical, and genetic. An integrated in silico screening strategy for identifying. Using a protein interaction chip approach, we first established the global tp53 and tp63 interaction network comprising of 383 and 301 proteins, respectively. The p53 tetramer shows an inducedfit interaction of the c. This application provides tools to mine, filter, and view p53 cistrome data in table format, and with hierarchical clustering of the filtered results. Dual regulation of p53 by the ribosome maturation factor. The new tp53 website has been launched with a novel design, updated information and improved readability. We employed prism 64,65 to screen 54 different potential interaction partners for the p53.
Dnabinding protects p53 from interactions with cofactors. Identification of new inhibitors of mdm2p53 interaction. Revealing a human p53 universe nucleic acids research. Qsar models for isoindolinonebased p53mdm2 interaction.
In addition, the structure of the recently reported spirooxindole inhibitor bound to mdm2 is described. The iarc tp53 database compiles various types of data and information on human tp53 gene variations related to cancer. The model with the highest scoring of fakntand p53 peptide interaction. Despite the extensive validation of this strategy, there are relatively few crystallographically determined cocomplex structures for smallmolecular inhibitors of the mdm2 p53 interaction. The affinity of p53 for specific binding sites relative to other dna sequences is an. Structure based virtual screening, docking and molecular. Xray structures of mdm2 in complex with some ligands are available in protein data bank and herein, these data have been exploited to efficiently identify new p53mdm2 interaction antagonists through a hierarchical virtual screening strategy. Thus, the study of the p53 pathway and its interaction networks is a promising source of insight for discovering therapeutic targets for tp53mutated cancers. Metaanalysis of the p53 mutation database for mutant p53 biological activity. The umd tp53 mutation database includes the tp53 status of more than 80,400 tumors, individuals with germline mutations and cell lines.
The p53 mutation database consists of a list of point mutations in the p53 gene of human tumors and cell lines, compiled from the published literature and made available through electronic media. The p53 database was set up in 1991 and the first publication of the database in 1992 contained 300 mutations 5. Since the 1997 release of the p53 database, a large number of changes have come about both in the database itself and in the software used to manage it 1,6,7. As a member of the wwpdb, the rcsb pdb curates and annotates pdb data according to agreed upon standards. The binding of p53 to sites that lack a p53 motif could result from a variety of factors, including p53 interactions. Rapid identification of dual p53mdm2mdmx interaction. Lexisnexis keeps improving interaction and offers firms a great way to develop stronger relationships with clients, prospects and referral sources. Staining of p53 and parp1 in breast cancer tmas and comparison with the tcga database indicated a higher doublepositive signal in basallike breast cancer than in luminal a or luminal b subtypes.
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