Novel mutations in <i>Lrp6</i> orthologs in mouse and human neural tube defects affect a highly dosage-sensitive Wnt non-canonical planar cell polarity pathway

Allache, Redouane; Lachance, Stéphanie; Guyot, Marie Claude; Marco, Patrizia De; Merello, Elisa; Justice, Monica J.; Capra, Valeria; Kibar, Zoha

doi:10.1093/hmg/ddt558

Cited by 36 publications

(48 citation statements)

References 49 publications

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“…Furthermore, there may be a biochemical connection between the Wnt/β-catenin and Wnt/PCP pathways in facilitating neural tube closure. While the LRP6 receptor is generally thought to be dedicated to Wnt/β-catenin signaling, recent data show that NTD-associated LRP6 mutations decrease Wnt/β-catenin activity while simultaneously increasing Wnt/PCP activity [58]. This supports the notion that these seemingly separable Wnt pathways engage in reciprocal inhibition and other forms of cross talk to form integrated signaling networks involved in developmental decision-making [13,61].…”

Section: Neural Plate Specification and Neural Tube Formationmentioning

confidence: 71%

“…A role for the Wnt/β-catenin pathway is indicated in this process as well. For example, mice with LOF mutations in either Axin1 or Tcf3 exhibit incomplete neural tube closure [53,54], and various mutations in LRP6 cause NTDs in mice [55,56,57], and are present in human NTD patients [58,59]. Recent evidence suggests defects in this case may be due in part to inappropriate fate specification of the laterally placed neural plate border cells governed by the Wnt/β-catenin pathway [60].…”

Section: Neural Plate Specification and Neural Tube Formationmentioning

confidence: 99%

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Neurodevelopmental Perspectives on Wnt Signaling in Psychiatry

Mulligan

Cheyette

2016

Complex Psychiatry

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Mounting evidence indicates that Wnt signaling is relevant to pathophysiology of diverse mental illnesses including schizophrenia, bipolar disorder, and autism spectrum disorder. In the 35 years since Wnt ligands were first described, animal studies have richly explored how downstream Wnt signaling pathways affect an array of neurodevelopmental processes and how their disruption can lead to both neurological and behavioral phenotypes. Recently, human induced pluripotent stem cell (hiPSC) models have begun to contribute to this literature while pushing it in increasingly translational directions. Simultaneously, large-scale human genomic studies are providing evidence that sequence variation in Wnt signal pathway genes contributes to pathogenesis in several psychiatric disorders. This article reviews neurodevelopmental and postneurodevelopmental functions of Wnt signaling, highlighting mechanisms, whereby its disruption might contribute to psychiatric illness, and then reviews the most reliable recent genetic evidence supporting that mutations in Wnt pathway genes contribute to psychiatric illness. We are proponents of the notion that studies in animal and hiPSC models informed by the human genetic data combined with the deep knowledge base and tool kits generated over the last several decades of basic neurodevelopmental research will yield near-term tangible advances in neuropsychiatry.

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Section: Neural Plate Specification and Neural Tube Formationmentioning

confidence: 71%

Section: Neural Plate Specification and Neural Tube Formationmentioning

confidence: 99%

Neurodevelopmental Perspectives on Wnt Signaling in Psychiatry

Mulligan

Cheyette

2016

Complex Psychiatry

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“…Another possibility is that the activities of the canonical Wnt and the PCP pathways are interdependent. For example, a hypermorphic allele of the canonical Wnt coreceptor lipoprotein receptor-related protein, Lrp6, increased Wnt canonical and, simultaneously, abolished PCP-induced JNK activities [117]. Several proteins have been shown to act as molecular switches between the Wnt/ -catenin and PCP signaling pathways [116,118] lending credibility to this mechanism.…”

Section: Planar Cell Polarity Pathway and Kidneymentioning

confidence: 99%

“…Indeed, several recent publications presented convincing data documenting antagonistic relationship between Wnt/ -catenin activity and PCP signaling [117,118]. The inv/inv mouse has cystic kidneys and laterality defects (situs inversus) [141], and knockdown of inv in zebrafish leads to a shortened anterior-posterior axis and widened somites, a classical manifestation of defective PCP signaling.…”

Section: Advances In Nephrologymentioning

confidence: 99%

Planar Cell Polarity Pathway in Kidney Development and Function

Rocque

Torban

2015

Advances in Nephrology

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The evolutionarily conserved planar cell polarity (PCP) signaling pathway controls tissue polarity within the plane orthogonal to the apical-basal axis. PCP was originally discovered in Drosophila melanogaster where it is required for the establishment of a uniform pattern of cell structures and appendages. In vertebrates, including mammals, the PCP pathway has been adapted to control various morphogenetic processes that are critical for tissue and organ development. These include convergent extension (crucial for neural tube closure and cochlear duct development) and oriented cell division (needed for tubular elongation), ciliary tilting that enables directional fluid flow, and other processes. Recently, strong evidence has emerged to implicate the PCP pathway in vertebrate kidney development. In this review, we will describe the experimental data revealing the role of PCP signaling in nephrogenesis and kidney disease.

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“…The wild‐type DIVERSIN open reading frame was cloned in pCDNA3.1 Myc/His A and the human mutations were introduced in this backbone by in site‐directed mutagenesis. The effect of the DIVERSIN variants on PCP signaling and on canonical Wnt/β catenin signaling was tested using the AP1 responsive JNK reporter assay (PathDetect Kit, Stratagene) and the TCF/LEF‐1 responsive Wnt/β‐catenin assay using the TOPFLASH /pGL3‐OT in mammalian HEK cells respectively as previously described (Allache et al, ). Briefly, HEK cells were transfected with (100 ng pAP1‐Luc, 300 ng pSV‐β‐Galactosidase, and 100 ng wild‐type or mutant DIVERSIN or empty pCDNA3.1 vector alone as control) DNA/well in 24‐well plates.…”

Section: Methodsmentioning

confidence: 99%