Literature DB >> 28805809

X-ray structures of endothelin ETB receptor bound to clinical antagonist bosentan and its analog.

Wataru Shihoya1,2,3, Tomohiro Nishizawa3,4, Keitaro Yamashita5, Asuka Inoue4,6, Kunio Hirata4,5, Francois Marie Ngako Kadji6, Akiko Okuta2, Kazutoshi Tani2, Junken Aoki6,7, Yoshinori Fujiyoshi1,2, Tomoko Doi8, Osamu Nureki3.   

Abstract

Endothelin receptors (ETRs) have crucial roles in vascular control and are targets for drugs designed to treat circulatory-system diseases and cancer progression. The nonpeptide dual-ETR antagonist bosentan is the first oral drug approved to treat pulmonary arterial hypertension. Here we report crystal structures of human endothelin ETB receptor bound to bosentan and to the ETB-selective analog K-8794, at 3.6-Å and 2.2-Å resolution, respectively. The K-8794-bound structure reveals the detailed water-mediated hydrogen-bonding network at the transmembrane core, which could account for the weak negative allosteric modulation of ETB by Na+ ions. The bosentan-bound structure reveals detailed interactions with ETB, which are probably conserved in the ETA receptor. A comparison of the two structures shows unexpected similarity between antagonist and agonist binding. Despite this similarity, bosentan sterically prevents the inward movement of transmembrane helix 6 (TM6), and thus exerts its antagonistic activity. These structural insights will facilitate the rational design of new ETR-targeting drugs.

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Year:  2017        PMID: 28805809     DOI: 10.1038/nsmb.3450

Source DB:  PubMed          Journal:  Nat Struct Mol Biol        ISSN: 1545-9985            Impact factor:   15.369


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