TY - JOUR
T1 - High-resolution structures of multiple 5-HT3aR-setron complexes reveal a novel mechanism of competitive inhibition
AU - Basak, Sandip
AU - Kumar, Arvind
AU - Ramsey, Steven
AU - Gibbs, Eric
AU - Kapoor, Abhijeet
AU - Filizola, Marta
AU - Chakrapani, Sudha
N1 - Funding Information:
Department of Ophthalmology and Visual Sciences (supported by the National Institutes of
Funding Information:
1548562. This work was supported by the National Institutes of Health grants R01GM108921,
Funding Information:
MCB080077 (to M.F.), which is supported by National Science Foundation grant number ACI-
Publisher Copyright:
© 2020, eLife Sciences Publications Ltd. All rights reserved.
PY - 2020/10
Y1 - 2020/10
N2 - Serotonin receptors (5-HT3AR) play a crucial role in regulating gut movement, and are the principal target of setrons, a class of high-affinity competitive antagonists, used in the management of nausea and vomiting associated with radiation and chemotherapies. Structural insights into setron-binding poses and their inhibitory mechanisms are just beginning to emerge. Here, we present high-resolution cryo-EM structures of full-length 5-HT3AR in complex with palonosetron, ondansetron, and alosetron. Molecular dynamic simulations of these structures embedded in a fully-hydrated lipid environment assessed the stability of ligand-binding poses and drug-target interactions over time. Together with simulation results of apo-and serotonin-bound 5-HT3AR, the study reveals a distinct interaction fingerprint between the various setrons and binding-pocket residues that may underlie their diverse affinities. In addition, varying degrees of conformational change in the setron-5-HT3AR structures, throughout the channel and particularly along the channel activation pathway, suggests a novel mechanism of competitive inhibition.
AB - Serotonin receptors (5-HT3AR) play a crucial role in regulating gut movement, and are the principal target of setrons, a class of high-affinity competitive antagonists, used in the management of nausea and vomiting associated with radiation and chemotherapies. Structural insights into setron-binding poses and their inhibitory mechanisms are just beginning to emerge. Here, we present high-resolution cryo-EM structures of full-length 5-HT3AR in complex with palonosetron, ondansetron, and alosetron. Molecular dynamic simulations of these structures embedded in a fully-hydrated lipid environment assessed the stability of ligand-binding poses and drug-target interactions over time. Together with simulation results of apo-and serotonin-bound 5-HT3AR, the study reveals a distinct interaction fingerprint between the various setrons and binding-pocket residues that may underlie their diverse affinities. In addition, varying degrees of conformational change in the setron-5-HT3AR structures, throughout the channel and particularly along the channel activation pathway, suggests a novel mechanism of competitive inhibition.
UR - http://www.scopus.com/inward/record.url?scp=85095611215&partnerID=8YFLogxK
U2 - 10.7554/eLife.57870
DO - 10.7554/eLife.57870
M3 - Article
C2 - 33063666
AN - SCOPUS:85095611215
SN - 2050-084X
VL - 9
SP - 1
EP - 56
JO - eLife
JF - eLife
M1 - e57870
ER -