TY - JOUR
T1 - Crystal Structures of Human Orexin 2 Receptor Bound to the Subtype-Selective Antagonist EMPA
AU - Suno, Ryoji
AU - Kimura, Kanako Terakado
AU - Nakane, Takanori
AU - Yamashita, Keitaro
AU - Wang, Junmei
AU - Fujiwara, Takaaki
AU - Yamanaka, Yasuaki
AU - Im, Dohyun
AU - Horita, Shoichiro
AU - Tsujimoto, Hirokazu
AU - Tawaramoto, Maki S.
AU - Hirokawa, Takatsugu
AU - Nango, Eriko
AU - Tono, Kensuke
AU - Kameshima, Takashi
AU - Hatsui, Takaki
AU - Joti, Yasumasa
AU - Yabashi, Makina
AU - Shimamoto, Keiko
AU - Yamamoto, Masaki
AU - Rosenbaum, Daniel M.
AU - Iwata, So
AU - Shimamura, Tatsuro
AU - Kobayashi, Takuya
N1 - Funding Information:
We thank Dr. Kunio Hirata for helping with the data collection at SPring-8. We acknowledge support from the Adaptable and Seamless Technology Transfer Program through target-driven R&D (A-STEP) funded by the Strategic Basic Research Program , Japan Science and Technology Agency (JST) (T. Kobayashi), the Research Acceleration Program of the JST (S.I.), Toray Science Foundation (T. Kobayashi), Takeda Science Foundation (T. Kobayashi and R.S.), the Naito Foundation (T. Kobayashi), the Platform for Drug Discovery, Informatics, and Structural Life Science (PDIS) funded by the Ministry of Education, Culture, Sports, Science and Technology (MEXT) of Japan (T. Kobayashi), the X-ray Free-Electron Laser Priority Strategy Program (MEXT) (T.S., S.I.), JSPS KAKENHI (grant nos. 26102725 , 15H04338 , and 17K19349 to T.S.; grant no. 15K08268 to R.S.; grant no. 15H06862 to K.Y.), and grant I-1770 from the Welch Foundation (D.R.). We thank Dr. Katsutoshi Sasaki at Kyowa Hakko Kirin and Prof. Masashi Yanagisawa at University of Tsukuba for their helpful discussion, Prof. Makoto Suematsu at Keio University for arrangement of EMPA synthesis, the beamline staff at SPring-8, and beamline staff at SACLA for data collection. We are grateful for the computational support from the SACLA HPC system and Mini-K super computer system. The X-ray crystallographic data collection was performed at SPring-8 (proposal no. 2013A1379, 2013B1092, 2013B1184, 2014A1301, 2014B1273, 2014B1355, 2015A1044, 2015A1080, 2015B2044, and 2015B2080) and SACLA (proposal no. 2013A8040, 2013B8044, 2014A8031, and 2015A8031).
Publisher Copyright:
© 2017 Elsevier Ltd
PY - 2018/1/2
Y1 - 2018/1/2
N2 - 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-Å and 1.96-Å 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 structures in complex with selective antagonists and previously determined OX1R/OX2R structures bound to non-selective antagonists revealed that the residue at positions 2.61 and 3.33 were critical for the antagonist selectivity in OX2R. The importance of these residues for binding selectivity to OX2R was also revealed by molecular dynamics simulation. These results should facilitate the development of antagonists for orexin receptors. Molecular dynamics simulations and structural information for orexin receptors indicates that the residues at positions 2.61 and 3.33 are critical for antagonist selectivity. Suno et al. determine the structure of a human GPCR using SACLA, and characterize differences between XFEL and synchrotron.
AB - 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-Å and 1.96-Å 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 structures in complex with selective antagonists and previously determined OX1R/OX2R structures bound to non-selective antagonists revealed that the residue at positions 2.61 and 3.33 were critical for the antagonist selectivity in OX2R. The importance of these residues for binding selectivity to OX2R was also revealed by molecular dynamics simulation. These results should facilitate the development of antagonists for orexin receptors. Molecular dynamics simulations and structural information for orexin receptors indicates that the residues at positions 2.61 and 3.33 are critical for antagonist selectivity. Suno et al. determine the structure of a human GPCR using SACLA, and characterize differences between XFEL and synchrotron.
KW - GPCR
KW - X-ray crystallography
KW - X-ray free-electron laser
KW - orexin receptor
KW - serial femtosecond crystallography
KW - subtype selective ligand
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U2 - 10.1016/j.str.2017.11.005
DO - 10.1016/j.str.2017.11.005
M3 - Article
C2 - 29225076
AN - SCOPUS:85039856148
SN - 0969-2126
VL - 26
SP - 7-19.e5
JO - Structure with Folding & design
JF - Structure with Folding & design
IS - 1
ER -