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Ligand recognition and activation of neuromedin U receptor 2.

Wenli ZhaoWenru ZhangMu WangMinmin LuShutian ChenTingting TangGisela SchnappHolger WagnerAlbert BrennauerCuiying YiXiaojing ChuShuo HanBeili WuQiang Zhao
Published in: Nature communications (2022)
Neuromedin U receptor 2 (NMU2), an emerging attractive target for treating obesity, has shown the capability in reducing food intake and regulating energy metabolism when activated. However, drug development of NMU2 was deferred partially due to the lack of structural information. Here, we present the cryo-electron microscopy (cryo-EM) structure of NMU2 bound to the endogenous agonist NmU-25 and G i1 at 3.3 Å resolution. Combined with functional and computational data, the structure reveals the key factors that govern the recognition and selectivity of peptide agonist as well as non-peptide antagonist, providing the structural basis for design of novel and highly selective drugs targeting NMU2. In addition, a 25-degree rotation of G i protein in reference to NMU2 is also observed compared in other structures of class A GPCR-G i complexes, suggesting heterogeneity in the processes of G protein-coupled receptors (GPCRs) activation and G protein coupling.
Keyphrases
  • electron microscopy
  • structural basis
  • high resolution
  • type diabetes
  • metabolic syndrome
  • insulin resistance
  • weight loss
  • healthcare
  • single cell
  • skeletal muscle
  • ionic liquid
  • deep learning
  • drug induced