Co-Located Conference AgendasFlow Chemistry Europe |  Other Track AgendasChemical Biology | Formulation and Solubility | Fragment Based Lead Discovery | Targeting Protein-Protein Interactions |
Tuesday, 19 March 201308:00 | Registration | |
Therapeutic Applications | Session Sponsors |
| | 09:00 |  | Keynote Presentation Targeting Protein-protein Interaction Between FOXM1 and NPM in Cancer
Andrei Gartel, Associate Professor, University of Illinois at Chicago, United States of America
FOXM1 and NPM are over-expressed in human cancers. NPM interacts with FOXM1 and their interaction is required for sustaining the level and localization of FOXM1. Targeting the interaction between FOXM1 and NPM may represent a novel therapeutic strategy against cancer. |
| 10:00 | Targeting Bivalent Menin-MLL Interaction in Leukemia with Small Molecule Inhibitors
Tomasz Cierpicki, Assistant Professor, University of Michigan, United States of America
In this presentation we will discuss development of potent small molecules inhibiting the protein-protein interaction between menin and MLL. These inhibitors demonstrate very potent and specific effects in targeting oncogenic activity of MLL fusion proteins in leukemia. | 10:30 | Coffee Break and Networking in the Exhibition Hall | 11:15 | Robust Three-dimensional Tools to Design Inhibitors Against Drug Targets Which Lack Explicit Specificity
Moses Prabu, Group Leader, Protein Sciences, Berg Pharma, United States of America
The design of robust drugs that specifically block targets with promiscuous binding specificity is a major challenge for structure-based drug design. Our substrate-envelope approach provides new insights for designing novel inhibitors for targets that are capable of recognizing chemically diverse ligands. | |
Novel Tools Applied to Protein-Protein Interaction |
| | 11:45 | Approaches to the Discovery of Small-molecule MDM2-p53 Inhibitors
Ian Hardcastle, Lecturer, Newcastle University, United Kingdom
The MDM2-p53 protein-protein interaction is a well validated and tractable drug target. Potent small-molecule inhibitors including the Nutlin series have been reported. The approaches for the discovery of MDM2-p53 inhibitors based on the isoindolinone, and pyrrole scaffold will be described. | 12:15 | Lunch and Networking in Exhibition Hall | 13:30 | Poster Viewing Session | 14:15 | CANCELLED - Protein Docking and Conformational Properties of the Interfaces
Ilya Vakser, Professor, The University of Kansas, United States of America
New methodology for structural modeling of PPI is based on rapidly increasing knowledge of protein complexes. The approach is designed for atomic resolution prediction of protein interfaces and assessment of their druggability. | 14:45 | An ACE Method for Monitoring Protein-protein Interactions (PPIs)
Carol Austin, Group Leader, Selcia Limited, United Kingdom
Affinity capillary electrophoresis (ACE) can readily detect protein-protein interactions in solution, without the need to immobilise protein. The technique is able to detect weak affinity fragments. Examples of ACE PPI assays will be presented. | 15:15 | Coffee Break and Networking in the Exhibition Hall | 16:00 | Library Design for Tackling Protein-protein Interactions: The 2P2I Approach
Philippe Roche, Senior Scientist, National Center for Scientific Research, France
We have developed 2P2IDB, a hand-curated structural database dedicated to PPI with known orthosteric inhibitors. Using structural knowledge from the recent success stories our goal is to derive some common principles to help future target selection by assessing the druggability of PPI and to accelerate the process of drug discovery by improving the quality of chemical libraries dedicated to PPI. | 16:30 | CANCELLED - Biophotonic Nanoswitches to Control Cell Fate
Rudolf Allemann, Distinguished Research Professor, Cardiff University, United Kingdom
Specific recognition of one protein by another is a fundamental biological mechanism for the regulation of cellular pathways with opportunities for the development of precision research tools and medicines. We have created reversible biophotonic nanoswitches that control commitment to apoptosis. | 16:30 | Computational Approaches For The Discovery Of Small Molecule Protein-Protein Interaction Inhibitors
Arnout Voet, Researcher, RIKEN, Japan
First, we will focus on the computational methodology for the discovery of Small Molecule Protien-Protien Interaction Inhibitors (SMPPIIs). Then we focus on 2 different cases in which we were successful for the discovery of first in class SMPPII for new PPI targets. | 17:00 | End of Day One |
Wednesday, 20 March 2013 |
Protein-protein Interaction in Disease and Drug Development |
| | 09:30 |  | Keynote Presentation Interacting with Protein Interactions
Arthur Olson, Professor, The Scripps Research Institute, United States of America
Understanding the complex nature of protein interactions, especially in the context of cellular environments, requires new tools and approaches to visualization, interaction and software development. We present and demonstrate some of our recent work in this area. |
| 10:30 | Coffee Break and Networking in the Exhibition Hall | 11:15 | Protein Surface Recogntion by Calixarenes - Assembly and Camouflage
Peter Crowley, Professor, National University of Ireland Galway, Ireland
Controlled protein assembly is one of the cornerstones of bionanotechnology. This talk focuses on the use of small molecule mediators to drive protein assembly. Two examples involving sulfonatocalixarene will be presented. The concept of protein camouflage will also be discussed. | 11:45 | Druggability of Dynamic Protein-protein Interfaces
Volkhard Helms, Chair of Computational Biology, Universitat des Saarlandes, Germany
Molecular dynamics simulations of the proteins MDM2, IL-2, Bcl-XL, the XIAP Bir2 domain, and PDK1 identified frequent formation of transition pockets on the protein surfaces. Ligand docking confirmed that these pockets are suitable to bind known ligand molecules. | 12:15 | Lunch and Networking in Exhibition Hall | 13:30 | Poster Viewing Session | 14:15 | The Convergence of Mechanistic Targets for Neurodegeneration and Cancer
James Bibb, Associate Professor, University of Texas Southwestern Medical Center, United States of America
The molecular processes that mediate synaptic remodeling required for cognition and neuronal injury appear to share many mechanisms that in non-neuronal populations of cells can induce neoplasia. Evidence in the form of animal models and signal transduction pathways demonstrating this link and the validation of common mechanistic targets for drug discovery will be presented.
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Post Translational Modifications |
| | 14:45 | Inhibition of Protein-protein Interactions Using Designed Molecules
Andrew Wilson, Reader in Synthetic Chemistry, University of Leeds, United Kingdom
This presentation will describe the design and synthesis of (i) oligoamide based a-helix mimetics and (ii) highly functionalised ruthenium tris(bipyridine) complexes, together with their use as inhibitors of a-helix mediated PPIs and receptors for solvent exposed protein surfaces respectively. | 15:15 | Coffee Break and Networking in the Exhibition Hall | 15:45 | The Development of Stapled Peptides that Modulate the BRCA2-RAD51 Interaction
Chiara Valenzano, Post-Doctoral Researcher, University of Cambridge, United Kingdom
The interaction between the human recombinase RAD51 and the hub protein BRCA2 is crucial for the repair of double strand breaks via homologous DNA recombination. We designed and validated stapled peptides as chemical tools to unravel mechanistic aspects of this protein-protein interaction. | 16:45 | Close of Conference |
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