The polarity protein Pard3 is required for centrosome positioning during neurulation

Microtubules are essential regulators of cell polarity, architecture and motility. The organization of the microtubule network is context-specific. In non-polarized cells, microtubules are anchored to the centrosome and form radial arrays. In most epithelial cells, microtubules are noncentrosomal, a...

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Published inDevelopmental biology Vol. 341; no. 2; pp. 335 - 345
Main Authors Hong, Elim, Jayachandran, Pradeepa, Brewster, Rachel
Format Journal Article
LanguageEnglish
Published United States Elsevier Inc 15.05.2010
Subjects
Animals
Axoneme - metabolism
Carrier Proteins - analysis
Carrier Proteins - metabolism
Cell Polarity
Centrosome
Centrosome - metabolism
Cilia
Cilia - metabolism
Cytoskeleton
Danio rerio
Mesenchymal–epithelial transition
Microtubules
Microtubules - metabolism
Neural tube
Neurulation
Pard3
Zebrafish
Zebrafish - embryology
Zebrafish Proteins - analysis
Zebrafish Proteins - metabolism
Neural tube
Pard3
Microtubules
Mesenchymal–epithelial transition
Zebrafish
Cytoskeleton
Cell polarity
Centrosome
Cilia
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Summary:Microtubules are essential regulators of cell polarity, architecture and motility. The organization of the microtubule network is context-specific. In non-polarized cells, microtubules are anchored to the centrosome and form radial arrays. In most epithelial cells, microtubules are noncentrosomal, align along the apico-basal axis and the centrosome templates a cilium. It follows that cells undergoing mesenchyme-to-epithelium transitions must reorganize their microtubule network extensively, yet little is understood about how this process is orchestrated. In particular, the pathways regulating the apical positioning of the centrosome are unknown, a central question given the role of cilia in fluid propulsion, sensation and signaling. In zebrafish, neural progenitors undergo progressive epithelialization during neurulation, and thus provide a convenient in vivo cellular context in which to address this question. We demonstrate here that the microtubule cytoskeleton gradually transitions from a radial to linear organization during neurulation and that microtubules function in conjunction with the polarity protein Pard3 to mediate centrosome positioning. Pard3 depletion results in hydrocephalus, a defect often associated with abnormal cerebrospinal fluid flow that has been linked to cilia defects. These findings thus bring to focus cellular events occurring during neurulation and reveal novel molecular mechanisms implicated in centrosome positioning.
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ISSN:0012-1606
1095-564X
DOI:10.1016/j.ydbio.2010.01.034