QSAR METHODS DEVELOPMENT, VIRTUAL AND EXPERIMENTAL SCREENING FOR CANNABINOID LIGAND DISCOVERY

G protein coupled receptors (GPCRs) are the largest receptor family in mammalian genomes and are known to regulate wide variety of signals such as ions, hormones and neurotransmitters. It has been estimated that GPCRs represent more than 30% of current drug targets and have attracted many pharmaceutical industries as well as academic groups for potential drug discovery. Cannabinoid (CB) receptors, members of GPCR superfamily, are also involved in the activation of multiple intracellular signal transductions and their endogenous ligands or cannabinoids have attracted pharmacological research because of their potential therapeutic effects. In particular, the cannabinoid subtype-2 (CB2) receptor is known to be involved in immune system signal transductions and its ligands have the potential to be developed as drugs to treat many immune system disorders without potential psychotic side-effects. Therefore, this work was focused on discovering novel CB2 ligands by developing novel quantitative structure-activity relationship (QSAR) methods and performing virtual and experimental screenings. Three novel QSAR methods were developed to predict biological activities and binding affinities of ligands. In the first method, a traditional fragment-based approach was improved by introducing a fragment similarity concept that enhanced the prediction accuracy remarkably. In the second method, pharmacophoric and morphological descriptors were incorporated to derive a novel QSAR regression model with good prediction accuracy. In the third method, a novel fingerprint-based artificial neural network QSAR model was developed to overcome the similar scaffold requirement of many fragment-based and other 3D-QSAR methods. These methods provide a foundation for virtual screening and hit ranking of chemical ligands from large chemical space. In addition, several novel CB2 selective ligands within nM binding affinities were discovered. These ligands were proven to be inverse agonists as validated by functional assays and could be useful probes to study CB2 signaling as well as potential drug candidates for autoimmune disesases

Targeting tumors using peptides

To penetrate solid tumors, low molecular weight (Mw < 10 KDa) compounds have an edge over antibodies: their higher penetration because of their small size. Because of the dense stroma and high interstitial fluid pressure of solid tumors, the penetration of higher Mw compounds is unfavored and being small thus becomes an advantage. This review covers a wide range of peptidic ligands—linear, cyclic, macrocyclic and cyclotidic peptides—to target tumors: We describe the main tools to identify peptides experimentally, such as phage display, and the possible chemical modifications to enhance the properties of the identified peptides. We also review in silico identification of peptides and the most salient non-peptidic ligands in clinical stages. We later focus the attention on the current validated ligands available to target different tumor compartments: blood vessels, extracelullar matrix, and tumor associated macrophages. The clinical advances and failures of these ligands and their therapeutic conjugates will be discussed. We aim to present the reader with the state-of-the-art in targeting tumors, by using low Mw molecules, and the tools to identify new ligands.Fil: Scodeller, Pablo David. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. University of Tartu; EstoniaFil: Asciutto, Eliana Karina. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Universidad Nacional de San Martín. Escuela de Ciencia y Tecnología; Argentin