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Tubulin detyrosination promotes monolayer formation and apical trafficking in epithelial cells
31
Citations
50
References
2012
Year
CytoskeletonCellular PhysiologyMonolayer FormationTubulin TyrosinationTubulin DetyrosinationTubulin Tyrosine LigaseCell SignalingCell PhysiologyCell PolarityCell TraffickingMembrane BiologyProtein TransportCell BiologyApical TraffickingDevelopmental BiologyIntracellular TransportIntracellular TraffickingCellular BiochemistryCellular StructureMedicineExtracellular Matrix
The role of post-translational tubulin modifications in the development and maintenance of a polarized epithelium is not well understood. We studied the balance between detyrosinated (detyr-) and tyrosinated (tyr-) tubulin in the formation of MDCK cell monolayers. Increased quantities of detyrosinated microtubules were detected during assembly into confluent cell sheets. These tubules were composed of alternating stretches of detyr- and tyr-tubulin. Constant induction of tubulin tyrosination, which decreased the levels of detyr-tubulin by overexpression of tubulin tyrosine ligase (TTL), disrupted monolayer establishment. Detyr-tubulin-depleted cells assembled into isolated islands and developed a prematurely polarized architecture. Thus, tubulin detyrosination is required for the morphological differentiation from non-polarized cells into an epithelial monolayer. Moreover, membrane trafficking, in particular to the apical domain, was slowed down in TTL-overexpressing cells. This effect could be reversed by TTL knockdown, which suggests that detyr-tubulin-enriched microtubules serve as cytoskeletal tracks to guide membrane cargo in polarized MDCK cells.
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