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

Valnohová, Jana; Kowalski-Jahn, Maria; Sunahara, Roger K.; Schulte, Gunnar

doi:10.1074/jbc.ra118.004763

Cited by 20 publications

(18 citation statements)

References 60 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Several amino residuals in intracellular loops 1, 2, and 3 and the flanking region near to intracellular loop 3 were also important for the intracellular location of Dishevelled while the mutant impaired the binding of Dishevelled [73–77]. Research based on FZD6 also showed that the linker domain, especially some conserved cystines, between the CRD domain and seven transmembrane core was imperative for Dishevelled recruitment [78]. One potential mechanism for FZD4 activation would be a Wnt/Norrin-induced movement of the seventh transmembrane domain to expose the key FZD4-Dishevelled interaction site [79].…”

Section: Resultsmentioning

confidence: 99%

Familial Exudative Vitreoretinopathy-Related Disease-Causing Genes and Norrin/β-Catenin Signal Pathway: Structure, Function, and Mutation Spectrums

Xiao

Tong

Zhu

et al. 2019

Journal of Ophthalmology

View full text Add to dashboard Cite

Familial exudative vitreoretinopathy (FEVR) is a hereditary ocular disorder characterized by incomplete vascularization/abnormality of peripheral retina. Four of the identified disease-causing genes of FEVR were NDP, FZD4, LRP5, and TSPAN12, the protein coded by which were the components of the Norrin/β-catenin signal pathway. In this review, we summarized and discussed the spectrum of mutations involving these four genes. By the end of 2017, the number of FEVR causing mutations reported for NDP, FZD4, LRP5, and TSPAN12 was, respectively, 26, 121, 58, and 40. Three most frequently reported mutations were c. 362G > A (p.R121Q) of NDP, c. 313A > G (p.M105V), and c.1282_1285delGACA (p.D428SfsX2) of FZD4. Mutations have a tendency to cluster in some “hotspots” domains which may be responsible for protein interactions.

show abstract

Section: Resultsmentioning

confidence: 99%

Familial Exudative Vitreoretinopathy-Related Disease-Causing Genes and Norrin/β-Catenin Signal Pathway: Structure, Function, and Mutation Spectrums

Xiao

Tong

Zhu

et al. 2019

Journal of Ophthalmology

View full text Add to dashboard Cite

show abstract

“…DVL is a central mediator of the β-catenin-dependent and PCP-like WNT signaling pathways and its recruitment to FZD is an initial step in DVL-dependent signaling 12,47,48 . Simultaneous overexpression of DVL and FZD leads to FZD-dependent membrane recruitment of DVL even in the absence of a ligand [49][50][51] colocalization and recruitment of cytosolic DVL present in punctate aggregates to membrane-expressed FZDs 47,[49][50][51] . However, quantification of recruitment and measurement of ligandinduced dynamics were not possible.…”

Section: Sag13 Affects Fzd 6 -Dvl2mentioning

confidence: 99%

“…In order to assess ligand-induced effects on DVL-FZD BRET, we chose an acceptor:donor ratio corresponding to the plateau part of the saturation curves for both setups. In addition, we did not treat the cells with the porcupine inhibitor C59 to block secretion of endogenous WNTs as their presence had no significant effect on the basal recruitment of the overexpressed DVL2 to the overexpressed FZD 6 as recently reported 51 and presented in Supplementary Fig. 15a, b.…”

Section: Sag13 Affects Fzd 6 -Dvl2mentioning

confidence: 99%

“…FLAG-FZD 6 -Nluc and ΔCRD FLAG-FZD 6 -Nluc were subcloned from FLAG-FZD 6 -His and ΔCRD FLAG-FZD 6 -His, respectively, into pNluc-N1 with BgIII and AgeI. SNAP-FZD 6 -Rluc8, SNAP-FZD 7 -Rluc8, SMO-Rluc8, Nluc-DVL2, FLAG-FZD 6 -His, ΔCRD FLAG-FZD 6 -His, and FZD 4 -Nluc were generated and validated in our previous studies 15,51 .…”

Section: Cloning Of Receptor Constructs and Mutagenesis Nluc-a 3 Wasmentioning

confidence: 99%

See 1 more Smart Citation

Structural insight into small molecule action on Frizzleds

et al. 2020

Self Cite

View full text Add to dashboard Cite

WNT-Frizzled (FZD) signaling plays a critical role in embryonic development, stem cell regulation and tissue homeostasis. FZDs are linked to severe human pathology and are seen as a promising target for therapy. Despite intense efforts, no small molecule drugs with distinct efficacy have emerged. Here, we identify the Smoothened agonist SAG1.3 as a partial agonist of FZD 6 with limited subtype selectivity. Employing extensive in silico analysis, resonance energy transfer-and luciferase-based assays we describe the mode of action of SAG1.3. We define the ability of SAG1.3 to bind to FZD 6 and to induce conformational changes in the receptor, recruitment and activation of G proteins and dynamics in FZD-Dishevelled interaction. Our results provide the proof-of-principle that FZDs are targetable by small molecules acting on their seven transmembrane spanning core. Thus, we provide a starting point for a structure-guided and mechanism-based drug discovery process to exploit the potential of FZDs as therapeutic targets.

show abstract

“…For example, it is still a mystery how the phosphoprotein dishevelled (DVL), which acts as a central signalling relay and FZD‐interacting scaffold in several β‐catenin‐dependent and β‐catenin‐independent WNT signalling pathways, biochemically mediates WNT‐induced and FZD‐mediated signal initiation and transmission – despite its polymerization in agonist‐induced signalosomes. Further, it remains unclear, if DVL interaction with FZDs is weakened or strengthened upon agonist stimulation in the light of conflicting findings . In this context, it remains obscure if DVL could act as a FZD binding partner to form a ternary complex in a pharmacological sense as previously hypothesized .…”

Section: Introductionmentioning

confidence: 95%

Structural insight into Class F receptors – What have we learnt regarding agonist‐induced activation?

Schulte

Kozielewicz

2019

Basic Clin Pharma Tox

Self Cite

View full text Add to dashboard Cite

Class F receptors, including the ten Frizzleds (FZD 1-10 ) and SMO, mediate the effects of WNTs and hedgehog proteins and belong to the superfamily of G proteincoupled receptors (GPCRs). While the recent, high-resolution insight into mechanisms of GPCR activation provides a better understanding of receptor activation in Class A, B and C GPCRs, it remains unclear how Class F receptors bind their ligands, how ligand binding is translated to receptor activation and how signal initiation and specification are achieved. Here, we summarize recent efforts in elucidating Class F receptor structure and activation mechanisms and critically discuss the progress made in this area. A better understanding of the activation mechanisms of Class F receptors is required to engage in mechanism-based and structure-guided drug discovery to exploit the large therapeutic potential of targeting these receptors pharmacologically.

show abstract

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

Cited by 20 publications

References 60 publications

Familial Exudative Vitreoretinopathy-Related Disease-Causing Genes and Norrin/β-Catenin Signal Pathway: Structure, Function, and Mutation Spectrums

Familial Exudative Vitreoretinopathy-Related Disease-Causing Genes and Norrin/β-Catenin Signal Pathway: Structure, Function, and Mutation Spectrums

Structural insight into small molecule action on Frizzleds

Structural insight into Class F receptors – What have we learnt regarding agonist‐induced activation?

Contact Info

Product

Resources

About