A PTK7/Ror2 Co-Receptor Complex Affects Xenopus Neural Crest Migration.

Neural crest cells are a highly migratory pluripotent cell population that generates a wide array of different cell types and failure in their migration can result in severe birth defects and malformation syndromes. Neural crest migration is controlled by various means including chemotaxis, repellen...

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Main Authors: Martina Podleschny, Anita Grund, Hanna Berger, Erik Rollwitz, Annette Borchers
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4683079?pdf=render
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spelling doaj-6dca4c223a9f4d039330ae813c5aeeba2020-11-25T02:31:24ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-011012e014516910.1371/journal.pone.0145169A PTK7/Ror2 Co-Receptor Complex Affects Xenopus Neural Crest Migration.Martina PodleschnyAnita GrundHanna BergerErik RollwitzAnnette BorchersNeural crest cells are a highly migratory pluripotent cell population that generates a wide array of different cell types and failure in their migration can result in severe birth defects and malformation syndromes. Neural crest migration is controlled by various means including chemotaxis, repellent guidance cues and cell-cell interaction. Non-canonical Wnt PCP (planar cell polarity) signaling has previously been shown to control cell-contact mediated neural crest cell guidance. PTK7 (protein tyrosine kinase 7) is a transmembrane pseudokinase and a known regulator of Wnt/PCP signaling, which is expressed in Xenopus neural crest cells and required for their migration. PTK7 functions as a Wnt co-receptor; however, it remains unclear by which means PTK7 affects neural crest migration. Expressing fluorescently labeled proteins in Xenopus neural crest cells we find that PTK7 co-localizes with the Ror2 Wnt-receptor. Further, co-immunoprecipitation experiments demonstrate that PTK7 interacts with Ror2. The PTK7/Ror2 interaction is likely relevant for neural crest migration, because Ror2 expression can rescue the PTK7 loss of function migration defect. Live cell imaging of explanted neural crest cells shows that PTK7 loss of function affects the formation of cell protrusions as well as cell motility. Co-expression of Ror2 can rescue these defects. In vivo analysis demonstrates that a kinase dead Ror2 mutant cannot rescue PTK7 loss of function. Thus, our data suggest that Ror2 can substitute for PTK7 and that the signaling function of its kinase domain is required for this effect.http://europepmc.org/articles/PMC4683079?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Martina Podleschny
Anita Grund
Hanna Berger
Erik Rollwitz
Annette Borchers
spellingShingle Martina Podleschny
Anita Grund
Hanna Berger
Erik Rollwitz
Annette Borchers
A PTK7/Ror2 Co-Receptor Complex Affects Xenopus Neural Crest Migration.
PLoS ONE
author_facet Martina Podleschny
Anita Grund
Hanna Berger
Erik Rollwitz
Annette Borchers
author_sort Martina Podleschny
title A PTK7/Ror2 Co-Receptor Complex Affects Xenopus Neural Crest Migration.
title_short A PTK7/Ror2 Co-Receptor Complex Affects Xenopus Neural Crest Migration.
title_full A PTK7/Ror2 Co-Receptor Complex Affects Xenopus Neural Crest Migration.
title_fullStr A PTK7/Ror2 Co-Receptor Complex Affects Xenopus Neural Crest Migration.
title_full_unstemmed A PTK7/Ror2 Co-Receptor Complex Affects Xenopus Neural Crest Migration.
title_sort ptk7/ror2 co-receptor complex affects xenopus neural crest migration.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description Neural crest cells are a highly migratory pluripotent cell population that generates a wide array of different cell types and failure in their migration can result in severe birth defects and malformation syndromes. Neural crest migration is controlled by various means including chemotaxis, repellent guidance cues and cell-cell interaction. Non-canonical Wnt PCP (planar cell polarity) signaling has previously been shown to control cell-contact mediated neural crest cell guidance. PTK7 (protein tyrosine kinase 7) is a transmembrane pseudokinase and a known regulator of Wnt/PCP signaling, which is expressed in Xenopus neural crest cells and required for their migration. PTK7 functions as a Wnt co-receptor; however, it remains unclear by which means PTK7 affects neural crest migration. Expressing fluorescently labeled proteins in Xenopus neural crest cells we find that PTK7 co-localizes with the Ror2 Wnt-receptor. Further, co-immunoprecipitation experiments demonstrate that PTK7 interacts with Ror2. The PTK7/Ror2 interaction is likely relevant for neural crest migration, because Ror2 expression can rescue the PTK7 loss of function migration defect. Live cell imaging of explanted neural crest cells shows that PTK7 loss of function affects the formation of cell protrusions as well as cell motility. Co-expression of Ror2 can rescue these defects. In vivo analysis demonstrates that a kinase dead Ror2 mutant cannot rescue PTK7 loss of function. Thus, our data suggest that Ror2 can substitute for PTK7 and that the signaling function of its kinase domain is required for this effect.
url http://europepmc.org/articles/PMC4683079?pdf=render
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