作者
Tao Che, Susruta Majumdar, Saheem A Zaidi, Pauline Ondachi, John D McCorvy, Sheng Wang, Philip D Mosier, Rajendra Uprety, Eyal Vardy, Brian E Krumm, Gye Won Han, Ming-Yue Lee, Els Pardon, Jan Steyaert, Xi-Ping Huang, Ryan T Strachan, Alexandra R Tribo, Gavril W Pasternak, F Ivy Carroll, Raymond C Stevens, Vadim Cherezov, Vsevolod Katritch, Daniel Wacker, Bryan L Roth
发表日期
2018/1/11
期刊
Cell
卷号
172
期号
1
页码范围
55-67. e15
出版商
Elsevier
简介
The κ-opioid receptor (KOP) mediates the actions of opioids with hallucinogenic, dysphoric, and analgesic activities. The design of KOP analgesics devoid of hallucinatory and dysphoric effects has been hindered by an incomplete structural and mechanistic understanding of KOP agonist actions. Here, we provide a crystal structure of human KOP in complex with the potent epoxymorphinan opioid agonist MP1104 and an active-state-stabilizing nanobody. Comparisons between inactive- and active-state opioid receptor structures reveal substantial conformational changes in the binding pocket and intracellular and extracellular regions. Extensive structural analysis and experimental validation illuminate key residues that propagate larger-scale structural rearrangements and transducer binding that, collectively, elucidate the structural determinants of KOP pharmacology, function, and biased signaling. These …
引用总数
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