Ligand Recognition in μ Opioid Receptor: Experimentally Based Modeling of μ Opioid Receptor Binding Sites and Their Testing by Ligand Docking

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• 作者：Sagara ; Takeshi ; Egashira ; Hiromu ; Okamura ; Mikako ; Fujii ; Ikuo ; Shimohigashi ; Yasuyuki ; Kanematsu ; Ken
• 刊名：Bioorganic and Medicinal Chemistry
• 出版年：1996
• 出版时间：December, 1996
• 年：1996
• 卷：4
• 期：1
• 页码：2151-2166
• 全文大小：1.15 M

文摘

For three-dimensional understanding of the mechanisms that control potency and selectivity of the ligand binding at the atomic level, we have analysed opioid receptor-ligand interaction based on the receptor's 3D model. As a first step, we have constructed molecular models for the multiple opioid receptor subtypes using bacteriorhodopsin as a template. The S-activated dihydromorphine derivatives should serve as powerful tools in mapping the three-dimensional structure of the μ opioid receptor, including the nature of the agonist-mediated conformational change that permits G protein-coupling to ‘second messenger’ effector molecules, and in identifying specific ligand-binding contacts with the μ opioid receptor. The analyses of the interactions of some opioid ligands with the predicted ligand binding sites are consistent with the results of the affinity labeling experiments.