Contractile forces at tricellular contacts modulate epithelial organization and monolayer integrity

三细胞接触处的收缩力调节上皮细胞的组织结构和单层完整性。

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作者:Julie Salomon ,Cécile Gaston ,Jérémy Magescas ,Boris Duvauchelle ,Danielle Canioni ,Lucie Sengmanivong ,Adeline Mayeux ,Grégoire Michaux ,Florence Campeotto ,Julie Lemale ,Jérôme Viala ,Françoise Poirier ,Nicolas Minc ,Jacques Schmitz ,Nicole Brousse ,Benoit Ladoux ,Olivier Goulet ,Delphine Delacour

Abstract

Monolayered epithelia are composed of tight cell assemblies that ensure polarized exchanges. EpCAM, an unconventional epithelial-specific cell adhesion molecule, is assumed to modulate epithelial morphogenesis in animal models, but little is known regarding its cellular functions. Inspired by the characterization of cellular defects in a rare EpCAM-related human intestinal disease, we find that the absence of EpCAM in enterocytes results in an aberrant apical domain. In the course of this pathological state, apical translocation towards tricellular contacts (TCs) occurs with striking tight junction belt displacement. These unusual cell organization and intestinal tissue defects are driven by the loss of actomyosin network homoeostasis and contractile activity clustering at TCs, yet is reversed by myosin-II inhibitor treatment. This study reveals that adequate distribution of cortical tension is crucial for individual cell organization, but also for epithelial monolayer maintenance. Our data suggest that EpCAM modulation protects against epithelial dysplasia and stabilizes human tissue architecture.

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