| Literature DB >> 30135577 |
Shifan Yang1, Yiran Wu1, Ting-Hai Xu2, Parker W de Waal2, Yuanzheng He3, Mengchen Pu1, Yuxiang Chen1,4,5,6, Zachary J DeBruine2, Bingjie Zhang1, Saheem A Zaidi7, Petr Popov7,8, Yu Guo1,4,5,6, Gye Won Han7, Yang Lu3, Kelly Suino-Powell2, Shaowei Dong1,4,5,6, Kaleeckal G Harikumar9, Laurence J Miller9, Vsevolod Katritch7,8, H Eric Xu2,10, Wenqing Shui1,4, Raymond C Stevens1,4, Karsten Melcher2, Suwen Zhao1,4, Fei Xu11,12.
Abstract
Frizzled receptors (FZDs) are class-F G-protein-coupled receptors (GPCRs) that function in Wnt signalling and are essential for developing and adult organisms1,2. As central mediators in this complex signalling pathway, FZDs serve as gatekeeping proteins both for drug intervention and for the development of probes in basic and in therapeutic research. Here we present an atomic-resolution structure of the human Frizzled 4 receptor (FZD4) transmembrane domain in the absence of a bound ligand. The structure reveals an unusual transmembrane architecture in which helix VI is short and tightly packed, and is distinct from all other GPCR structures reported so far. Within this unique transmembrane fold is an extremely narrow and highly hydrophilic pocket that is not amenable to the binding of traditional GPCR ligands. We show that such a pocket is conserved across all FZDs, which may explain the long-standing difficulties in the development of ligands for these receptors. Molecular dynamics simulations on the microsecond timescale and mutational analysis uncovered two coupled, dynamic kinks located at helix VII that are involved in FZD4 activation. The stability of the structure in its ligand-free form, an unfavourable pocket for ligand binding and the two unusual kinks on helix VII suggest that FZDs may have evolved a novel ligand-recognition and activation mechanism that is distinct from that of other GPCRs.Entities:
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Year: 2018 PMID: 30135577 DOI: 10.1038/s41586-018-0447-x
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962