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Wong, Hing C.; Mao, Junhao; Nguyen, Jason; Srinivas, Shamala; Zhang, Weixing; Liu, Bo; Li, Lin; Wu, Dianqing; Zheng, Jie

doi:10.1038/82047

Cited by 132 publications

(29 citation statements)

References 49 publications

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“…2b). The existence of this short helix has already been postulated and shown to be involved in the interaction of Fz4 with the effector protein Dishevelled1527, while the remaining part of the wt tail (from Leu 511 to Val 537 ) was predicted to be disordered27. We judged the structure prediction for the mutant tail sound and worthwhile of further experimental proof.…”

Section: Resultsmentioning

confidence: 83%

“…Two PDZ binding motives are located one internally and one at the C-terminus of Fz4. The cytosolic tail of Fz4 has been shown to interact with the protein Dishevelled to activate several signalling pathways141516. The frameshift mutation L501fsX533 of Fz4 is associated with a rare form of Familial exudative vitreorethinopaty (FEVR)17 that shows an autosomal dominant inheritance.…”

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confidence: 99%

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A disorder-to-order structural transition in the COOH-tail of Fz4 determines misfolding of the L501fsX533-Fz4 mutant

Lemma

D’Agostino

Caporaso

et al. 2013

Sci Rep

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Frizzled 4 belongs to the superfamily of G protein coupled receptors. The unstructured cytosolic tail of the receptor is essential for its activity. The mutation L501fsX533 in the fz4 gene results in a new COOH-tail of the receptor and causes a form of Familial exudative vitreoretinopathy. Here we show that the mutated tail is structured. Two amphipathic helices, displaying affinity for membranes and resembling the structure of Influenza Hemagglutinin fusion peptide, constitute the new fold. This tail induces the aggregation of the receptor in the Endoplasmic Reticulum and it is sufficient to block the export to the Golgi of a chimeric VSVG protein containing the mutated tail. Affecting the tail's structure, net charge or amphipathicity relocates the mutated Fz4 receptor to the Plasma Membrane. Such disorder-to-order structural transition was never described in GPCRs and opens a new scenario on the possible effect of mutations on unstructured regions of proteins.

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Section: Resultsmentioning

confidence: 83%

mentioning

confidence: 99%

A disorder-to-order structural transition in the COOH-tail of Fz4 determines misfolding of the L501fsX533-Fz4 mutant

Lemma

D’Agostino

Caporaso

et al. 2013

Sci Rep

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“…However, our data indicate that it is the Lysine itself that is essential and a mutation to the related Arginine residue (which is similarly charged and often can substitute for Lys) also causes the same defects as the original DshK417M mutation. These data suggest that it is a post-translational modification such as ubiquitination or acetylation of Lys417, as it does not appear to be of structural importance (Wong et al, 2000). This notion is consistent with recent work in mammalian cell culture (Ganner et al, 2009), although we cannot exclude a direct involvement of Lys417.…”

Section: Discussionmentioning

confidence: 99%

Functional dissection of phosphorylation of Disheveled in Drosophila

Yanfeng

Berhane

Mola

et al. 2011

Developmental Biology

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Dishevelled/Dsh proteins (Dvl in mammals) are core components of both Wnt/Wg-signaling pathways: canonical β-catenin signaling and Frizzled (Fz)-planar cell polarity (PCP) signaling. Although Dsh is a key cytoplasmic component of both Wnt/Fz-pathways, regulation of its signaling specificity is not well understood. Dsh is phosphorylated, but the functional significance of its phosphorylation remains unclear. We have systematically investigated the phosphorylation of Dsh by combining mass-spectrometry analyses, biochemical studies, and in vivo genetic methods in Drosophila. Our approaches identified multiple phospho-residues of Dsh in vivo. Our data define three novel and unexpected conclusions: (1) Strikingly and in contrast to common assumptions, all conserved serines/threonines are non-essential for Dsh function in either pathway; (2) phosphorylation of conserved Tyrosine473 in the DEP domain is critical for PCP-signaling - DshY473F behaves like a PCP-specific allele; and (3) defects associated with the PCP specific dsh1 allele, DshK417M, located within a putative Protein Kinase C consensus site, are likely due to a post-translational modification requirement of Lys417, rather than phosphorylation nearby. In summary, our combined data indicate that while many Ser/Thr and Tyr residues are indeed phosphorylated in vivo, strikingly most of these phosphorylation events are not critical for Dsh function with the exception of DshY473.

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“…They function as essential scaffold proteins that interact with diverse proteins, including kinases, phosphatases, and adaptor proteins. They contain three highly conserved domains: the DIX (Disheveled/Axin) domain that is largely α-helical structure (Capelluto et al 2002), the PDZ (PSD-95, DLG,ZO1) domain, which consists of six β-sheets that enfold two α-helices (Wong et al 2003), and the DEP (Disheveled, EGL-10, Pleckstrin) domain, consisting of a bundle of three α-helices domain (Wong et al 2000). Several additional conserved regions are considered critical for biological function: the serine/threonine stretches between the DIX and PDZ domains, and the proline-rich regions with a SH3 protein-binding domain motif downstream of the PDZ.…”

Section: Introductionmentioning

confidence: 99%

Genetic Analysis of Disheveled 2 and Disheveled 3 in Human Neural Tube Defects

et al. 2012

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Neural tube defects are severe malformations affecting 1/1,000 live births. The planar cell polarity pathway controls the neural tube closure and has been implicated in the pathogenesis of neural tube defects both in animal models and human cohorts. In mouse disruption of Dvl2 alone (Dvl2−/−) or Dvl2 and Dvl3 (Dvl2−/−; Dvl3+/−, Dvl2+/−; Dvl3−/−) results in incomplete neurulation, suggesting a role for Disheveled in neural tube closure. Disheveled is a multifunctional protein that is involved in both the canonical Wnt signaling and the noncanonical planar cell polarity pathway. In this study, we analyzed the role of the human orthologs DVL2 and DVL3 in a cohort of 473 patients with neural tube defects. Rare variants were genotyped in 639 ethnically matched controls. We identified seven rare missense mutations that were absent in all controls analyzed. Two of these mutations, p.Tyr667Cys and p.Ala53Val, identified in DVL2 were predicted to be detrimental in silico. Significantly, a 1-bp insertion (c.1801_1802insG) in exon 15 of DVL2 predicted to lead to the truncation of the protein was identified in a patient with a complex form of caudal agenesis. In summary, we demonstrate a possible role for rare variants in DVL2 gene as risk factors for neural tube defects.Electronic supplementary materialThe online version of this article (doi:10.1007/s12031-012-9871-9) contains supplementary material, which is available to authorized users.

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Cited by 132 publications

References 49 publications

A disorder-to-order structural transition in the COOH-tail of Fz4 determines misfolding of the L501fsX533-Fz4 mutant

A disorder-to-order structural transition in the COOH-tail of Fz4 determines misfolding of the L501fsX533-Fz4 mutant

Functional dissection of phosphorylation of Disheveled in Drosophila

Genetic Analysis of Disheveled 2 and Disheveled 3 in Human Neural Tube Defects

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