Name: Workshop on Integrative modelling with HADDOCK in conjunction with Workshop on Novel Computational Methods for Structural Biology
Start: 2023-03-20T09:00:00+08:00
End: 2023-03-20T17:30:00+08:00
Location: BHSS, Academia Sinica

Workshop on Integrative modelling with HADDOCK in conjunction with Workshop on Novel Computational Methods for Structural Biology

Monday, 20 March 2023 - 09:00

Monday, 20 March 2023
09:00 General introduction to docking, integrative modelling and HADDOCK - Alexandre M.J.J. Bonvin (Utrecht University)
General introduction to docking, integrative modelling and HADDOCK
- Alexandre M.J.J. Bonvin (Utrecht University)
09:00 - 10:30
Room: Room 1
10:30 Coffee Break
Coffee Break
10:30 - 11:00
Room: Room 1
11:00 Computer practical: Antibody-antigen docking with the HADDOCK server - Alexandre M.J.J. Bonvin (Utrecht University)
Computer practical: Antibody-antigen docking with the HADDOCK server
- Alexandre M.J.J. Bonvin (Utrecht University)
11:00 - 12:30
Room: Room 1 HADDOCK2.4 antibody-antigen docking tutorial: This tutorial demonstrates the use of HADDOCK2.4 for predicting the structure of an antibody-antigen complex using information about the hypervariable loops of the antibody and either the entire surface of the antigen or a loose definition of the epitope. This tutorial does not require any Linux expertise and only makes use of our web servers and PyMol for visualisation/analysis. https://www.bonvinlab.org/education/HADDOCK24/HADDOCK24-antibody-antigen/
12:30 Lunch
Lunch
12:30 - 14:00
Room: Room 1
14:00 Lecture & practical: Introduction to HADDOCK3 and practical - Alexandre M.J.J. Bonvin (Utrecht University)
Lecture & practical: Introduction to HADDOCK3 and practical
- Alexandre M.J.J. Bonvin (Utrecht University)
14:00 - 15:30
Room: Room 1 HADDOCK3 antibody-antigen docking: This tutorial demonstrates the use of HADDOCK3 for predicting the structure of an antibody-antigen complex using information about the hypervariable loops of the antibody and either the entire surface of the antigen or a loose definition of the epitope. It illustrate the modularity of HADDOCK3 by introducing a new workflow not possible under the current HADDOCK2.X versions. As HADDOCK3 only exists as a command line version, this tutorial does require some basic Linux expertise. https://www.bonvinlab.org/education/HADDOCK3/HADDOCK3-antibody-antigen/
15:30 Coffee Break
Coffee Break
15:30 - 16:00
Room: Room 1
16:00
16:00 - 17:30
Room: Room 1
Contributions

16:00 Different Facets of Distance Geometry - Antonio MUCHERINO (Institut de Recherche en Informatique et Systèmes Aléatoires, University of Rennes 1, France)

16:30 A Curvilinear-Path Umbrella Sampling Approach to Characterizing Thermodynamics and Mechanisms of Biomolecular Interactions - Dhananjay JOSHI (Research Center for Applied Science, Academia Sinica)

17:00 Quantum Machine Learning for Structure-Based Virtual Screening of the Entire Medicinal Chemical Space - It has been estimated based on the graph theory that there are at least 1060 organic molecules that are relevant for small-molecule drug discovery. Using machine learning to estimate the binding free energies for screening of large chemical libraries to search for the tightly binding inhibitors would take a considerable amount of computational resources, yet it is not possible to explore the entire biologically relevant chemical space. Quantum computing provides a unique opportunity to accomplish such a computational task in the near future. Here, we demonstrate how to use 512 occupancies to describe the structures of protein-ligand complexes, how to convert the classical occupancies to the quantum states using nine qubits, and to estimate the binding free energies (Gbind) of the complexes using quantum machine learning. We showed that it is possible to use only 450 parameters to prepare the quantum states for describing the structure of one protein-ligand complex. In this work the entire 2020 PDBbind dataset was adopted as the training set, and we used 45 parameters as the first attempt to construct the model for predicting the binding free energies (Gbind). The Pearson correlation coefficient (PCC) between the estimated binding free energies and the corresponding experimental values are 0.49. By slightly increasing to 1,440 parameters for constructing the neural network model for the prediction of the Gbind, the PCC is improved to be 0.78, which is even slightly better than to the results achieved by recent classical convolutional neural network models using more than millions of parameters. In this work, for the first time, we demonstrated the feasibility of using quantum computers to explore the entire medicinal chemical space with a concrete, implementable approach. LIN (Research Center for Applied Science, Academia Sinica)