5-HT 2C Receptor Structures Reveal the Structural Basis of GPCR Polypharmacology

Journal:
Cell
Published:
DOI:
10.1016/j.cell.2018.01.001
Affiliations:
13
Authors:
20

Research Highlight

The path to more intelligent drug design

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A ShanghaiTech University-led team has revealed the structures of a serotonin receptor when bound to a polypharmacologic drug—one that binds to many receptors—and when bound to a selective drug. In doing so, they elucidated multiple receptor properties that may enable more intelligent drug design.

The team imaged a specific class of serotonin receptor, known as a 5-HT2c receptor, when bound to the polypharmacologic biomolecule ergotamine. By comparing the complex’s structure to other known ergotamine-complementary receptors, the researchers identified ten points of interaction that are highly conserved across many receptors and facilitate ergotamine binding.

In contrast, the drug ritanserin is selective towards the 5-HT2 family of serotonin receptors and, on examination, revealed a binding profile not found outside of the family.

The different changes induced in 5-HT2c by ergotamine and ritanserin indicate distinct signaling mechanisms that may inform future efforts into pathway-specific drugs.

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References

  1. Cell 172, 719–730 (2018). doi: 10.1016/j.cell.2018.01.001
Institutions Authors Share
ShanghaiTech University, China
6.333333
0.32
The University of North Carolina at Chapel Hill (UNC), United States of America (USA)
4.500000
0.23
University of Copenhagen (UCPH), Denmark
3.500000
0.18
University of Southern California (USC), United States of America (USA)
2.600000
0.13
Swiss Federal Institute of Technology Lausanne (EPFL), Switzerland
1.000000
0.05
National Laboratory of Biomacromolecules (NLB), IBP CAS, China
0.833333
0.04
NIMH Psychoactive Drug Screening Program (PDSP), United States of America (USA)
0.500000
0.03
Moscow Institute of Physics and Technology - State University (MIPT), Russia
0.400000
0.02
Kunming Medical University (KMU), China
0.333333
0.02