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Homology modeling and molecular docking studies of Drosophila and Aedes sex peptide receptors

  • Jeong Hyun Kim
  • , Soo Kyung Kim
  • , Jae Hyuk Lee
  • , Young Joon Kim
  • , William A. Goddard
  • , Yong Chul Kim
  • Gwangju Institute of Science and Technology
  • California Institute of Technology

Résultats de recherche: Contribution à un journalArticleRevue par des pairs

Résumé

The Drosophila melanogaster sex peptide receptor (DrmSPR), which is a G protein-coupled receptor (GPCR), is known as the specific receptor for sex peptide (SP). It is responsible for the reproductive behavior in the Drosophila model system; in particular, it is involved in the post-mating responses such as the increase in egg-laying ability and decrease in receptivity in females. In a previous study, we discovered a small molecule agonist of DrmSPR for the first time, which could not, however, activate Aedes aegypti SPR (AedesSPR). To investigate the binding mechanism of the small molecule agonist of DrmSPR, the ensemble structures of low-lying packing structures of DrmSPR and AedesSPR were assembled using the GEnSeMBLE (GPCR Ensemble of Structures in Membrane BiLayer Environment) method. The generated homology models exhibited the typical pattern of inter-helical interactions of the class A GPCRs. The docking experiments of the small molecule agonist suggest that Tyr5.35 and Phe2.67 residues may be involved in a hydrophobic interaction and that Ser3.25 forms a hydrogen bond with the agonist. Additionally, we found that the docking results were consistent with the experimental data of the reference compounds with variable agonistic activities. Moreover, a potential distinction of the putative binding sites in two GPCR models of DrmSPR and AedesSPR, which was determined in this study, can explain the selective action of the agonist for DrmSPR but not for AedesSPR.

langue originaleAnglais
Pages (de - à)115-122
Nombre de pages8
journalJournal of Molecular Graphics and Modelling
Volume66
Les DOIs
étatPublié - 1 mai 2016
Modification externeOui

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