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Crystal Structures of Human Orexin 2 Receptor Bound to the Subtype-Selective Antagonist EMPA.

Structure. 2018; 
Suno R, Kimura KT, Nakane T, Yamashita K, Wang J, Fujiwara T, Yamanaka Y, Im D, Horita S, Tsujimoto H, Tawaramoto MS, Hirokawa T, Nango E, Tono K, Kameshima T, Hatsui T, Joti Y, Yabashi M, Shimamoto K, Yamamoto M, Rosenbaum DM, Iwata S, Shimamura T, Kobayashi T.
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Codon Optimization abysii glycogen synthase (PGS) fusion construct was generated by synthetic DNA (GenScript).... The coding sequence of wild-type OX2R from residues 1 to 444 and the N-terminal HA-tag, FLAG tag sequence, 3C protease digestion site, C-terminal 3C protease site, and 10 3 His-tag was synthesized by optimization of codon usage for Sf9 cells (GenScript). Get A Quote

摘要

Orexin peptides in the brain regulate physiological functions such as the sleep-wake cycle, and are thus drug targets for the treatment of insomnia. Using serial femtosecond crystallography and multi-crystal data collection with a synchrotron light source, we determined structures of human orexin 2 receptor in complex with the subtype-selective?antagonist EMPA (N-ethyl-2-[(6-methoxy-pyridin-3-yl)-(toluene-2-sulfonyl)-amino]-N-pyridin-3-ylmethyl-acetamide) at 2.30-? and 1.96-? resolution. In comparison with the non-subtype-selective antagonist suvorexant, EMPA contacted fewer residues through hydrogen bonds at the orthosteric site, explaining the faster dissociation rate. Comparisons among these OX2R structur... More

關(guān)鍵詞

GPCR; X-ray crystallography; X-ray free-electron laser; orexin receptor; serial femtosecond crystallography; subtype selective ligand
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