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Structure of a nanobody-stabilized active state of the beta(2) adrenoceptor

Authors
Rasmussen, Soren G. F.Choi, Hee-JungFung, Juan JosePardon, ElsCasarosa, PaolaChae, Pil SeokDeVree, Brian T.Rosenbaum, Daniel M.Thian, Foon SunKobilka, Tong SunSchnapp, AndreasKonetzki, IngoSunahara, Roger K.Gellman, Samuel H.Pautsch, AlexanderSteyaert, JanWeis, William I.Kobilka, Brian K.
Issue Date
Jan-2011
Publisher
Nature Publishing Group
Citation
Nature, v.469, no.7329, pp.175 - 180
Indexed
SCIE
SCOPUS
Journal Title
Nature
Volume
469
Number
7329
Start Page
175
End Page
180
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/38304
DOI
10.1038/nature09648
ISSN
0028-0836
Abstract
G protein coupled receptors (GPCRs) exhibit a spectrum of functional behaviours in response to natural and synthetic ligands. Recent crystal structures provide insights into inactive states of several GPCRs. Efforts to obtain an agonist-bound active-state GPCR structure have proven difficult due to the inherent instability of this state in the absence of a G protein. We generated a camelid antibody fragment (nanobody) to the human beta(2) adrenergic receptor (beta(2)AR) that exhibits G protein-like behaviour, and obtained an agonist-bound, active-state crystal structure of the receptor-nanobody complex. Comparison with the inactive beta(2)AR structure reveals subtle changes in the binding pocket; however, these small changes are associated with an 11 angstrom outward movement of the cytoplasmic end of transmembrane segment 6, and rearrangements of transmembrane segments 5 and 7 that are remarkably similar to those observed in opsin, an active form of rhodopsin. This structure provides insights into the process of agonist binding and activation.
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COLLEGE OF ENGINEERING SCIENCES > DEPARTMENT OF BIONANO ENGINEERING > 1. Journal Articles

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ERICA 공학대학 (DEPARTMENT OF BIONANO ENGINEERING)
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