Lrp6 is required for convergent extension during Xenopus gastrulation

Wnt signaling regulates β-catenin-mediated gene transcription and planar cell polarity (PCP). The Wnt co-receptor, Lrp6, is required for signaling along the β-catenin arm. We show that Lrp6 downregulation (by morpholino injection) or overexpression in Xenopus embryos disrupts convergent extension,...

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Published inDevelopment (Cambridge) Vol. 134; no. 22; pp. 4095 - 4106
Main Authors Tahinci, Emilios, Thorne, Curtis A, Franklin, Jeffrey L, Salic, Adrian, Christian, Kelly M, Lee, Laura A, Coffey, Robert J, Lee, Ethan
Format Journal Article
LanguageEnglish
Published England The Company of Biologists Limited 01.11.2007
Subjects
Amino Acid Sequence
Animals
Animals, Genetically Modified
beta Catenin - genetics
beta Catenin - physiology
Body Patterning - genetics
Cell Polarity - genetics
Cells, Cultured
Embryo, Nonmammalian
Gastrulation - genetics
Gene Expression Regulation, Developmental
Humans
Low Density Lipoprotein Receptor-Related Protein-6
Mesoderm - metabolism
Models, Biological
Molecular Sequence Data
Receptors, LDL - genetics
Receptors, LDL - metabolism
Receptors, LDL - physiology
Sequence Homology, Amino Acid
Signal Transduction - genetics
Tissue Distribution
Wnt Proteins - genetics
Xenopus
Xenopus - embryology
Xenopus - genetics
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Summary:Wnt signaling regulates β-catenin-mediated gene transcription and planar cell polarity (PCP). The Wnt co-receptor, Lrp6, is required for signaling along the β-catenin arm. We show that Lrp6 downregulation (by morpholino injection) or overexpression in Xenopus embryos disrupts convergent extension, a hallmark feature of Wnt/PCP components. In embryos with decreased Lrp6 levels, cells of the dorsal marginal zone (DMZ), which undergoes extensive cellular rearrangements during gastrulation, exhibit decreased length:width ratios, decreased migration, and increased numbers of transient cytoplasmic protrusions. We show that Lrp6 opposes Wnt11 activity and localizes to the posterior edge of migrating DMZ cells and that Lrp6 downregulation enhances cortical and nuclear localization of Dsh and phospho-JNK, respectively. Taken together, these data suggest that Lrp6 inhibits Wnt/PCP signaling. Finally, we identify the region of the Lrp6 protein with Wnt/PCP activity to a stretch of 36 amino acids, distinct from regions required for Wnt/β-catenin signaling. We propose a model in which Lrp6 plays a critical role in the switch from Wnt/PCP to Wnt/β-catenin signaling.
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ISSN:0950-1991
1477-9129
DOI:10.1242/dev.010272