Human Family With Sequence Similarity 83 Member B (Fam83B); A Target Enabling Package

Human Family With Sequence Similarity 83 Member B (Fam83B); A Target Enabling Package

FAM83A-H are newly identified oncogenes characterised by a conserved DUF1669 domain. FAM83B can substitute for RAS to promote malignant transformation. Ablation of FAM83B or mutation of Lys230 inhibits malignant phenotypes, implicating FAM83B as potential therapeutic target. As part of this TEP, we...

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Hauptverfasser: Pinkas, Daniel M., Bufton, Joshua C., Fox, Alice E., Ruda, Gian Filippo, Talon, Romain, Krojer, Tobias, Bradley, Anthony R., Delft, Frank Von, Brennan, Paul E., Fulcher, Luke J., Bozatzi, Polyxeni, Tachi-Menson, Theresa, Wu, Kevin Z. L., Cummins, Timothy D., Dunbar, Karen, Shrestha, Sabin, Wood, Nicola T., Weidlich, Simone, Macartney, Thomas J., Joby Varghese, Gourlay, Robert, Campbell, David G., Hutchinson, Luke D., Vogt, Janis, Cooper, Fay, Dingwell, Kevin S., Smith, James C., Sapkota, Gopal P., Bullock, Alex N.
Format: Dataset
Sprache:eng
Schlagworte:
Cancer
Chemical Biology
Disease
Drug Discovery
Drug Target
FAM83B
Infectious Disease
Malaria
Metabolic Diseases
Neuro
Neurological Genetic Disorders
Neuropsychiatry
Oncology
Orphan Disease
Probe
Protein
Structural Genomics
Structure
Structure Discovery
Target Enabling Package
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Zusammenfassung:FAM83A-H are newly identified oncogenes characterised by a conserved DUF1669 domain. FAM83B can substitute for RAS to promote malignant transformation. Ablation of FAM83B or mutation of Lys230 inhibits malignant phenotypes, implicating FAM83B as potential therapeutic target. As part of this TEP, we solved the first crystal structures from the FAM83 family, including FAM83A and FAM83B. The structures of the DUF1669 domain reveal a phospholipase D-like fold lacking conservation of key catalytic residues. We deorphanise the FAM83 DUF1669 domain as a critical docking scaffold for binding of casein kinase 1 isoforms. Finally, using XChem fragment screening we report chemical fragments that bind to Lys230 in the central pocket of the DUF1669 and form starting points for potential drug development.
DOI:10.5281/zenodo.1342540