Publications by authors named "Daniel T D Jones"

Article Synopsis
  • Adhesion G protein-coupled receptor (aGPCR) signaling plays a crucial role in development and tissue homeostasis, yet its mechanisms are not fully understood across all types.
  • Researchers systematically evaluated the activities of all 33 aGPCRs using advanced assays and found that only about 50% displayed significant activation dependent on intramolecular tethered agonists.
  • The study revealed a strong preference for G protein signaling in aGPCRs and provided valuable insights for future research and therapeutic strategies targeting these receptors.
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Adhesion G Protein Coupled Receptors (aGPCRs) have evolved an activation mechanism to translate extracellular force into liberation of a tethered agonist (TA) to effect cell signalling. We report here that ADGRF1 can signal through all major G protein classes and identify the structural basis for a previously reported Gα preference by cryo-EM. Our structure shows that Gα preference in ADGRF1 may derive from tighter packing at the conserved F569 of the TA, altering contacts between TM helix I and VII, with a concurrent rearrangement of TM helix VII and helix VIII at the site of Gα recruitment.

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Objective: The mitochondrial pyruvate carrier (MPC) has emerged as a promising drug target for metabolic disorders, including non-alcoholic steatohepatitis and diabetes, metabolically dependent cancers and neurodegenerative diseases. A range of structurally diverse small molecule inhibitors have been proposed, but the nature of their interaction with MPC is not understood, and the composition of the functional human MPC is still debated. The goal of this study was to characterise the human MPC protein in vitro, to understand the chemical features that determine binding of structurally diverse inhibitors and to develop novel higher affinity ones.

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