AI Article Synopsis

  • Class A G protein-coupled receptors (GPCRs) are important for cell signaling and are major drug targets, yet over 60% of them remain untapped for therapeutic use.
  • Traditional GPCR drugs often have adverse effects, but biased signaling offers a new approach for discovering safer therapeutics by targeting specific receptor conformations.
  • The review outlines the landscape of GPCR-biased modulators, highlighting recent advancements, therapeutic relevance, and the variations in understanding their biological effects across different GPCR families.

Article Abstract

Class A G protein-coupled receptors (GPCRs) continue to garner interest for their essential roles in cell signalling and their importance as drug targets. Although numerous drugs in the clinic target these receptors, over 60% GPCRs remain unexploited. Moreover, the adverse effects triggered by the available unbiased GPCR modulators, limit their use and therapeutic value. In this context, the elucidation of biased signalling has opened up new pharmacological avenues holding promise for safer therapeutics. Functionally selective ligands favour receptor conformations facilitating the recruitment of specific effectors and the modulation of the associated pathways. This review surveys the current drug discovery landscape of GPCR-biased modulators with a focus on recent advances. Understanding the biological effects of this preferential coupling is at different stages depending on the Class A GPCR family. Therefore, with a focus on individual GPCR families, we present a compilation of the functionally selective modulators reported over the past few years. In doing so, we dissect their therapeutic relevance, molecular determinants and potential clinical applications.

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Source
http://dx.doi.org/10.1111/bph.17301DOI Listing

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