Literature DB >> 21807950

Analysis of protein dynamics within the septate junction reveals a highly stable core protein complex that does not include the basolateral polarity protein Discs large.

Kenzi Oshima1, Richard G Fehon.   

Abstract

Barrier junctions prevent pathogen invasion and restrict paracellular leakage across epithelial sheets. To understand how one barrier junction, the septate junction (SJ), is regulated in vivo, we used fluorescence recovery after photobleaching (FRAP) to examine SJ protein dynamics in Drosophila. Most SJ-associated proteins, including Coracle, Neurexin IV and Nervana 2, displayed similar, extremely immobile kinetics. Loss of any of these components resulted in dramatically increased mobility of all others, suggesting that they form a single, highly interdependent core complex. Immobilization of SJ core components coincided with formation of the morphological SJ but occurred after their known role in maintaining epithelial polarity, suggesting that these functions are independent. In striking contrast to the core components, the tumor suppressor protein Discs large was much more mobile and its loss did not affect mobility of core SJ proteins, suggesting that it is not a member of this complex, even though it colocalizes with the SJ. Similarly, disruption of endocytosis affected localization of SJ core components, but did not affect their mobility. These results indicate that formation of a stable SJ core complex is separable from its proper subcellular localization, and provide new insights into the complex processes that regulate epithelial polarity and assembly of the SJ.
© 2011. Published by The Company of Biologists Ltd

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Year:  2011        PMID: 21807950      PMCID: PMC3148133          DOI: 10.1242/jcs.087700

Source DB:  PubMed          Journal:  J Cell Sci        ISSN: 0021-9533            Impact factor:   5.285


  60 in total

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5.  The development of cellular junctions in the Drosophila embryo.

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8.  The claudin-like megatrachea is essential in septate junctions for the epithelial barrier function in Drosophila.

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9.  Neuroglian, Gliotactin, and the Na+/K+ ATPase are essential for septate junction function in Drosophila.

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Journal:  J Cell Biol       Date:  2003-06-02       Impact factor: 10.539

10.  Gliotactin, a novel marker of tricellular junctions, is necessary for septate junction development in Drosophila.

Authors:  Joost Schulte; Ulrich Tepass; Vanessa J Auld
Journal:  J Cell Biol       Date:  2003-06-02       Impact factor: 10.539

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  32 in total

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Review 3.  Neuronal immunoglobulin superfamily cell adhesion molecules in epithelial morphogenesis: insights from Drosophila.

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Journal:  Philos Trans R Soc Lond B Biol Sci       Date:  2020-08-24       Impact factor: 6.237

4.  RhoGAP68F controls transport of adhesion proteins in Rab4 endosomes to modulate epithelial morphogenesis of Drosophila leg discs.

Authors:  Beatriz Hernandez de Madrid; Lina Greenberg; Victor Hatini
Journal:  Dev Biol       Date:  2015-01-21       Impact factor: 3.582

5.  Macroglobulin complement-related encodes a protein required for septate junction organization and paracellular barrier function in Drosophila.

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6.  Distinct activities of Scrib module proteins organize epithelial polarity.

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7.  Scribble and Discs-large direct initial assembly and positioning of adherens junctions during the establishment of apical-basal polarity.

Authors:  Teresa T Bonello; Wangsun Choi; Mark Peifer
Journal:  Development       Date:  2019-11-21       Impact factor: 6.868

8.  The cAMP effector PKA mediates Moody GPCR signaling in Drosophila blood-brain barrier formation and maturation.

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9.  Ecdysone regulates the Drosophila imaginal disc epithelial barrier, determining the length of regeneration checkpoint delay.

Authors:  Danielle DaCrema; Rajan Bhandari; Faith Karanja; Ryunosuke Yano; Adrian Halme
Journal:  Development       Date:  2021-03-19       Impact factor: 6.868

10.  The Drosophila tricellular junction protein Gliotactin regulates its own mRNA levels through BMP-mediated induction of miR-184.

Authors:  Zohreh Sharifkhodaei; Mojgan Padash-Barmchi; Mary M Gilbert; Gayathri Samarasekera; Tudor A Fulga; David Van Vactor; Vanessa J Auld
Journal:  J Cell Sci       Date:  2016-02-16       Impact factor: 5.285

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