Unsaturated fatty acyl recognition by Frizzled receptors mediates dimerization upon Wnt ligand binding

Nile, Aaron H.; Mukund, Susmith; Stanger, Karen; Wang, Weiru; Hannoush, Rami N.

doi:10.1073/pnas.1618293114

Cited by 98 publications

(123 citation statements)

References 44 publications

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“…It is clear that the hydrophobic channel on the FZD CRD has a strong preference for binding fatty acids or other lipid-like molecules. Indeed, a recent crystal structure of the hFZD7 CRD showed the hydrophobic channel occupied by a fatty acid that originated in the cells used for protein expression – which do not overexpress a Wnt (Nile et al, 2017). In this study and another (DeBruine et al, 2017), it was further shown that binding of free fatty acids induces FZD-CRD oligomerization.…”

Section: Discussionmentioning

confidence: 99%

“…This structure confirmed that a conserved serine (S187 in xWnt8) is the only acylation site, and suggested that the S187-linked palmitoleoyl moiety plays a crucial role in FZD binding by occupying a hydrophobic channel on the CRD. This hydrophobic channel also binds free fatty acids in a manner thought to promote FZD oligomerization (DeBruine et al, 2017; Nile et al, 2017). Since all Wnts except WntD are predicted to be acylated at this conserved serine (Nile and Hannoush, 2016; Takada et al, 2006), it is thought that Wnts all engage and activate FZDs through such acylation-dependent interactions (Figure 1A).…”

Section: Introductionmentioning

confidence: 99%

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Non-acylated Wnts Can Promote Signaling

et al. 2019

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SUMMARY Wnts are a family of 19 extracellular ligands that regulate cell fate, proliferation and migration during metazoan embryogenesis and throughout adulthood. Wnts are acylated post-translationally at a conserved serine and bind the extracellular cysteine-rich domain (CRD) of Frizzled (FZD) seven-pass transmembrane receptors. Although crystal structures suggest that acylation is essential for Wnt binding to FZDs, we show here that several Wnts can promote signaling in Xenopus laevis and Danio rerio embryos – as well as in an in vitro cell culture model – without acylation. The non-acylated Wnts are expressed at similar levels to wild-type counterparts and retain CRD binding. By contrast, we find that certain other Wnts do require acylation for biological activity in Xenopus embryos – although not necessarily for FZD binding. Our data argue that acylation-dependence of Wnt activity is context-specific. They further suggest that acylation may underlie aspects of ligand/receptor selectivity and/or control other aspects of Wnt function.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Non-acylated Wnts Can Promote Signaling

et al. 2019

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“…The importance of the linker cysteines for receptor function is further underlined by previous reports identifying FZD 4 familial exudative vitreoretinopathy (FEVR) mutations in Cys-181 and Cys-204 of human FZD 4 (57)(58)(59). These C181R, C204R, C204Y mutations (corresponding to Cys-161 and Cys-185 in human FZD 6 , respectively) manifested with a trafficking phenotype and poor receptor surface expression (57,58).…”

Section: The Linker Domain Of Frizzledmentioning

confidence: 91%

“…FZDs, the focus of this study, bind WNT proteins with their extracellular cysteine-rich domain (CRD) to initiate a complex network of WNT signaling pathways (2). The CRD is seen as the orthosteric binding site for WNTs and is functionally implicated in receptor dimerization and signal initiation (3)(4)(5)(6). Structurally, the CRD is connected to the seven transmembrane (7TM) core of the receptor through a linker domain of variable length and low degree of conservation among the representatives of class F (5).…”

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confidence: 99%

Functional dissection of the N-terminal extracellular domains of Frizzled 6 reveals their roles for receptor localization and Dishevelled recruitment

Valnohová

Kowalski-Jahn

Sunahara

et al. 2018

Journal of Biological Chemistry

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The Frizzled (FZD) proteins belong to class F of G proteincoupled receptors (GPCRs) and are essential for various pathways involving the secreted lipoglycoproteins of the wingless/ int-1 (WNT) family. A WNT-binding cysteine-rich domain (CRD) in FZDs is N-terminally located and connected to the seven transmembrane domain-spanning receptor core by a linker domain that has a variable length in different FZD homologs. However, the function and importance of this linker domain are poorly understood. Here we used systematic mutagenesis of FZD 6 to define the minimal N-terminal domain sufficient for receptor surface expression and recruitment of the intracellular scaffold protein Dishevelled (DVL). Further, we identified a triad of evolutionarily conserved cysteines in the FZD linker domain that is crucial for receptor membrane expression and recruitment of DVL. Our results are in agreement with the concept that the conserved cysteines in the linker domain of FZDs assist with the formation of a common secondary structure in this region. We propose that this structure could be involved in agonist binding and receptor activation mechanisms that are similar to the binding and activation mechanisms known for other GPCRs.

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“…Furthermore, recent observations from the crystal structure of the Fzd7 CRD bound to a fatty acid has revealed that the palmitoleic lipid adduct binds to a U-shaped lipidbinding cavity of the Fzd7 dimer. Fzd5 and Fzd8 have similar architectures, including a dimeric arrangement of the CRD, suggesting a common model for how Wnt binds Fzd receptors via the fatty acid modification (Nile et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

Mechanisms of intercellular Wnt transport

2019

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Wnt proteins are secreted glycoproteins that regulate multiple processes crucial to the development and tissue homeostasis of multicellular organisms, including tissue patterning, proliferation, cell fate specification, cell polarity and migration. To elicit these effects, Wnts act as autocrine as well as paracrine signalling molecules between Wnt-producing and Wnt-receiving cells. More than 40 years after the discovery of the Wg/Wnt pathway, it is still unclear how they are transported to fulfil their paracrine signalling functions. Several mechanisms have been proposed to mediate intercellular Wnt transport, including Wnt-binding proteins, lipoproteins, exosomes and cytonemes. In this Review, we describe the evidence for each proposed mechanism, and discuss how they may contribute to Wnt dispersal in tissue-specific and context-dependent manners, to regulate embryonic development precisely and maintain the internal steady state within a defined tissue.

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Unsaturated fatty acyl recognition by Frizzled receptors mediates dimerization upon Wnt ligand binding

Cited by 98 publications

References 44 publications

Non-acylated Wnts Can Promote Signaling

Non-acylated Wnts Can Promote Signaling

Functional dissection of the N-terminal extracellular domains of Frizzled 6 reveals their roles for receptor localization and Dishevelled recruitment

Mechanisms of intercellular Wnt transport

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