In silico design of novel probes for the atypical opioid receptor MRGPRX2

نویسندگان

  • Katherine Lansu
  • Joel Karpiak
  • Jing Liu
  • Xi-Ping Huang
  • John D. McCorvy
  • Wesley K. Kroeze
  • Tao Che
  • Hiroshi Nagase
  • Frank I. Carroll
  • Jian Jin
  • Brian K. Shoichet
  • Bryan L. Roth
چکیده

The primate-exclusive MRGPRX2 G protein-coupled receptor (GPCR) has been suggested to modulate pain and itch. Despite putative peptide and small-molecule MRGPRX2 agonists, selective nanomolar-potency probes have not yet been reported. To identify a MRGPRX2 probe, we first screened 5,695 small molecules and found that many opioid compounds activated MRGPRX2, including (-)- and (+)-morphine, hydrocodone, sinomenine, dextromethorphan, and the prodynorphin-derived peptides dynorphin A, dynorphin B, and α- and β-neoendorphin. We used these to select for mutagenesis-validated homology models and docked almost 4 million small molecules. From this docking, we predicted ZINC-3573-a potent MRGPRX2-selective agonist, showing little activity against 315 other GPCRs and 97 representative kinases-along with an essentially inactive enantiomer. ZINC-3573 activates endogenous MRGPRX2 in a human mast cell line, inducing degranulation and calcium release. MRGPRX2 is a unique atypical opioid-like receptor important for modulating mast cell degranulation, which can now be specifically modulated with ZINC-3573.

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عنوان ژورنال:

دوره 13  شماره 

صفحات  -

تاریخ انتشار 2017