Litcius/Paper detail

Integration of Ligand-Based and Structure-Based Methods for the Design of Small-Molecule TLR7 Antagonists

Sourav Pal, Uddipta Ghosh Dastidar, Trisha Ghosh, Dipyaman Ganguly, Arindam Talukdar

2022Molecules16 citationsDOIOpen Access PDF

Abstract

Toll-like receptor 7 (TLR7) is activated in response to the binding of single-stranded RNA. Its over-activation has been implicated in several autoimmune disorders, and thus, it is an established therapeutic target in such circumstances. TLR7 small-molecule antagonists are not yet available for therapeutic use. We conducted a ligand-based drug design of new TLR7 antagonists through a concerted effort encompassing 2D-QSAR, 3D-QSAR, and pharmacophore modelling of 54 reported TLR7 antagonists. The developed 2D-QSAR model depicted an excellent correlation coefficient (R2training: 0.86 and R2test: 0.78) between the experimental and estimated activities. The ligand-based drug design approach utilizing the 3D-QSAR model (R2training: 0.95 and R2test: 0.84) demonstrated a significant contribution of electrostatic potential and steric fields towards the TLR7 antagonism. This consolidated approach, along with a pharmacophore model with high correlation (Rtraining: 0.94 and Rtest: 0.92), was used to design quinazoline-core-based hTLR7 antagonists. Subsequently, the newly designed molecules were subjected to molecular docking onto the previously proposed binding model and a molecular dynamics study for a better understanding of their binding pattern. The toxicity profiles and drug-likeness characteristics of the designed compounds were evaluated with in silico ADMET predictions. This ligand-based study contributes towards a better understanding of lead optimization and the future development of potent TLR7 antagonists.

Topics & Concepts

PharmacophoreQuantitative structure–activity relationshipIn silicoTLR7Computational biologyChemistryLigand (biochemistry)Docking (animal)Small moleculeDrugDrug discoveryRational designStereochemistryCombinatorial chemistryPharmacologyReceptorBiochemistryBiologyMedicineToll-like receptorGeneticsInnate immune systemNursingGeneImmune Response and InflammationVeterinary medicine and infectious diseasesAntimicrobial Peptides and Activities
Integration of Ligand-Based and Structure-Based Methods for the Design of Small-Molecule TLR7 Antagonists | Litcius