AI Article Synopsis

  • Researchers utilized cryo-electron microscopy (cryo-EM) to determine the full-length structure of the thyroid-stimulating hormone receptor (TSHR) complexed with a human monoclonal autoantibody K1-70™, a potent inhibitor of TSH action.
  • The TSHR was found to have a monomeric structure, displaying three domains: the leucine-rich domain (LRD), hinge region (HR), and transmembrane domain (TMD), with noticeable interactions between the TMD and the extracellular domain (ECD) that explain the effects of TSHR mutations.
  • The study also highlights how the binding of another stimulating autoantibody, M22™, may require the HR to rotate upwards to avoid cl

Article Abstract

Determination of the full-length thyroid-stimulating hormone receptor (TSHR) structure by cryo-electron microscopy (cryo-EM) is described. The TSHR complexed with human monoclonal TSHR autoantibody K1-70™ (a powerful inhibitor of TSH action) was detergent solubilised, purified to homogeneity and analysed by cryo-EM. The structure (global resolution 3.3 Å) is a monomer with all three domains visible: leucine-rich domain (LRD), hinge region (HR) and transmembrane domain (TMD). The TSHR extracellular domain (ECD, composed of the LRD and HR) is positioned on top of the TMD extracellular surface. Extensive interactions between the TMD and ECD are observed in the structure, and their analysis provides an explanation of the effects of various TSHR mutations on TSHR constitutive activity and on ligand-induced activation. K1-70™ is seen to be well clear of the lipid bilayer. However, superimposition of M22™ (a human monoclonal TSHR autoantibody which is a powerful stimulator of the TSHR) on the cryo-EM structure shows that it would clash with the bilayer unless the TSHR HR rotates upwards as part of the M22™ binding process. This rotation could have an important role in TSHR stimulation by M22™ and as such provides an explanation as to why K1-70™ blocks the binding of TSH and M22™ without activating the receptor itself.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9782461PMC
http://dx.doi.org/10.1530/JME-22-0120DOI Listing

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