Computational approaches for the characterization of the structure and dynamics of G Protein-Coupled Receptorsapplications to drug design

  1. Rodríguez Díaz, David
Dirixida por:
  1. Hugo Gutiérrez de Terán Castañón Director

Universidade de defensa: Universidade de Santiago de Compostela

Fecha de defensa: 09 de novembro de 2012

Tribunal:
  1. Leonardo Pardo Carrasco Presidente/a
  2. María de los Angeles Castro Pérez Secretaria
  3. Baldomero Oliva Miguel Vogal
  4. Chris de Graaf Vogal
  5. David Posada González Vogal

Tipo: Tese

Teseo: 336353 DIALNET

Resumo

G Protein-Coupled Receptors (GPCRs) constitute the most pharmacologically relevant superfamily of proteins. In this thesis, a computational pipeline for modelling the structure and dynamics of GPCRs is presented, properly combined with experimental collaborations for GPCR drug design. These include the discovery of novel scaffolds as potential antipsychotics, and the design of a new series of A3 adenosine receptor antagonists, employing successful combinations of structure- and ligand-based approaches. Additionally, the structure of Adenosine Receptors (ARs) was computationally assessed, with implications in ligand affinity and selectivity. The employed protocol for Molecular Dynamics simulations has allowed the characterization of structural determinants of the activation of ARs, and the evaluation of the stability of GPCR dimers of CXCR4 receptor. Finally, the computational pipeline here developed has been integrated into the web server GPCR-ModSim (http://gpcr.usc.es), contributing to its application in biochemical and pharmacological studies on GPCRs