Prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects

Planar cell polarity (PCP) is controlled by a conserved pathway that regulates directional cell behavior. Here, we show that mutant mice harboring a newly described mutation termed Beetlejuice (Bj) in Prickle1 (Pk1), a PCP component, exhibit developmental phenotypes involving cell polarity defects,...

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Autores principales: Gibbs, Brian C., Damerla, Rama Rao, Vladar, Eszter K., Chatterjee, Bishwanath, Wan, Yong, Liu, Xiaoqin, Cui, Cheng, Gabriel, George C., Zahid, Maliha, Yagi, Hisato, Szabo-Rogers, Heather L., Suyama, Kaye L., Axelrod, Jeffrey D., Lo, Cecilia W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists Ltd 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4810743/
https://www.ncbi.nlm.nih.gov/pubmed/26883626
http://dx.doi.org/10.1242/bio.015750
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author Gibbs, Brian C.
Damerla, Rama Rao
Vladar, Eszter K.
Chatterjee, Bishwanath
Wan, Yong
Liu, Xiaoqin
Cui, Cheng
Gabriel, George C.
Zahid, Maliha
Yagi, Hisato
Szabo-Rogers, Heather L.
Suyama, Kaye L.
Axelrod, Jeffrey D.
Lo, Cecilia W.
author_facet Gibbs, Brian C.
Damerla, Rama Rao
Vladar, Eszter K.
Chatterjee, Bishwanath
Wan, Yong
Liu, Xiaoqin
Cui, Cheng
Gabriel, George C.
Zahid, Maliha
Yagi, Hisato
Szabo-Rogers, Heather L.
Suyama, Kaye L.
Axelrod, Jeffrey D.
Lo, Cecilia W.
author_sort Gibbs, Brian C.
collection PubMed
description Planar cell polarity (PCP) is controlled by a conserved pathway that regulates directional cell behavior. Here, we show that mutant mice harboring a newly described mutation termed Beetlejuice (Bj) in Prickle1 (Pk1), a PCP component, exhibit developmental phenotypes involving cell polarity defects, including skeletal, cochlear and congenital cardiac anomalies. Bj mutants die neonatally with cardiac outflow tract (OFT) malalignment. This is associated with OFT shortening due to loss of polarized cell orientation and failure of second heart field cell intercalation mediating OFT lengthening. OFT myocardialization was disrupted with cardiomyocytes failing to align with the direction of cell invasion into the outflow cushions. The expression of genes mediating Wnt signaling was altered. Also noted were shortened but widened bile ducts and disruption in canonical Wnt signaling. Using an in vitro wound closure assay, we showed Bj mutant fibroblasts cannot establish polarized cell morphology or engage in directional cell migration, and their actin cytoskeleton failed to align with the direction of wound closure. Unexpectedly, Pk1 mutants exhibited primary and motile cilia defects. Given Bj mutant phenotypes are reminiscent of ciliopathies, these findings suggest Pk1 may also regulate ciliogenesis. Together these findings show Pk1 plays an essential role in regulating cell polarity and directional cell migration during development.
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spelling pubmed-48107432016-04-04 Prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects Gibbs, Brian C. Damerla, Rama Rao Vladar, Eszter K. Chatterjee, Bishwanath Wan, Yong Liu, Xiaoqin Cui, Cheng Gabriel, George C. Zahid, Maliha Yagi, Hisato Szabo-Rogers, Heather L. Suyama, Kaye L. Axelrod, Jeffrey D. Lo, Cecilia W. Biol Open Research Article Planar cell polarity (PCP) is controlled by a conserved pathway that regulates directional cell behavior. Here, we show that mutant mice harboring a newly described mutation termed Beetlejuice (Bj) in Prickle1 (Pk1), a PCP component, exhibit developmental phenotypes involving cell polarity defects, including skeletal, cochlear and congenital cardiac anomalies. Bj mutants die neonatally with cardiac outflow tract (OFT) malalignment. This is associated with OFT shortening due to loss of polarized cell orientation and failure of second heart field cell intercalation mediating OFT lengthening. OFT myocardialization was disrupted with cardiomyocytes failing to align with the direction of cell invasion into the outflow cushions. The expression of genes mediating Wnt signaling was altered. Also noted were shortened but widened bile ducts and disruption in canonical Wnt signaling. Using an in vitro wound closure assay, we showed Bj mutant fibroblasts cannot establish polarized cell morphology or engage in directional cell migration, and their actin cytoskeleton failed to align with the direction of wound closure. Unexpectedly, Pk1 mutants exhibited primary and motile cilia defects. Given Bj mutant phenotypes are reminiscent of ciliopathies, these findings suggest Pk1 may also regulate ciliogenesis. Together these findings show Pk1 plays an essential role in regulating cell polarity and directional cell migration during development. The Company of Biologists Ltd 2016-02-16 /pmc/articles/PMC4810743/ /pubmed/26883626 http://dx.doi.org/10.1242/bio.015750 Text en © 2016. Published by The Company of Biologists Ltd http://creativecommons.org/licenses/by/3.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0), which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Research Article
Gibbs, Brian C.
Damerla, Rama Rao
Vladar, Eszter K.
Chatterjee, Bishwanath
Wan, Yong
Liu, Xiaoqin
Cui, Cheng
Gabriel, George C.
Zahid, Maliha
Yagi, Hisato
Szabo-Rogers, Heather L.
Suyama, Kaye L.
Axelrod, Jeffrey D.
Lo, Cecilia W.
Prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects
title Prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects
title_full Prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects
title_fullStr Prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects
title_full_unstemmed Prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects
title_short Prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects
title_sort prickle1 mutation causes planar cell polarity and directional cell migration defects associated with cardiac outflow tract anomalies and other structural birth defects
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4810743/
https://www.ncbi.nlm.nih.gov/pubmed/26883626
http://dx.doi.org/10.1242/bio.015750
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