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Epithelial UNC-23 limits mechanical stress to maintain glia-neuron architecture in C. elegans
Journal article   Open access   Peer reviewed

Epithelial UNC-23 limits mechanical stress to maintain glia-neuron architecture in C. elegans

Cecilia G. Martin, James S. Bent, Tyler Hill, Irini Topalidou and Aakanksha Singhvi
Developmental cell, Vol.59(13), pp.1668-1688.e7
07/08/2024
PMID: 38670103

Abstract

Life Sciences & Biomedicine Science & Technology Cell Biology Developmental Biology
For an organ to maintain correct architecture and function, its diverse cellular components must coordinate their size and shape. Although cell-intrinsic mechanisms driving homotypic cell-cell coordination are known, it is unclear how cell shape is regulated across heterotypic cells. We find that epithelial cells maintain the shape of neighboring sense-organ glia-neuron units in adult Caenorhabditis elegans ( C. elegans ). Hsp cochaperone UNC-23/BAG2 prevents epithelial cell shape from deforming, and its loss causes head epithelia to stretch aberrantly during animal movement. In the sense-organ glia, amphid sheath (AMsh), this causes progressive fibroblast growth factor receptor (FGFR)-dependent disruption of the glial apical cytoskeleton. Resultant glial cell shape alteration causes concomitant shape change in glia-associated neuron endings. Epithelial UNC-23 maintenance of glia-neuron shape is specific both spatially, within a defined anatomical zone, and temporally, in a developmentally critical period. As all molecular components uncovered are broadly conserved across central and peripheral nervous systems, we posit that epithelia may similarly regulate glia-neuron architecture cross-species.
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https://doi.org/10.1016/j.devcel.2024.04.005View
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