Abstract
BackgroundThe development and homeostasis of multicellular organisms depends on sheets of epithelial cells. Bazooka (Baz; PAR-3) localizes to the apical circumference of epithelial cells and is a key hub in the protein interaction network regulating epithelial structure. We sought to identify additional proteins that function with Baz to regulate epithelial structure in the Drosophila embryo.Methodology/Principal FindingsThe baz zygotic mutant cuticle phenotype could be dominantly enhanced by loss of known interaction partners. To identify additional enhancers, we screened molecularly defined chromosome 2 and 3 deficiencies. 37 deficiencies acted as strong dominant enhancers. Using deficiency mapping, bioinformatics, and available single gene mutations, we identified 17 interacting genes encoding known and predicted polarity, cytoskeletal, transmembrane, trafficking and signaling proteins. For each gene, their loss of function enhanced adherens junction defects in zygotic baz mutants during early embryogenesis. To further evaluate involvement in epithelial polarity, we generated GFP fusion proteins for 15 of the genes which had not been found to localize to the apical domain previously. We found that GFP fusion proteins for Drosophila ASAP, Arf79F, CG11210, Septin 5 and Sds22 could be recruited to the apical circumference of epithelial cells. Nine of the other proteins showed various intracellular distributions, and one was not detected.Conclusions/SignificanceOur enhancer screen identified 17 genes that function with Baz to regulate epithelial structure in the Drosophila embryo. Our secondary localization screen indicated that some of the proteins may affect epithelial cell polarity by acting at the apical cell cortex while others may act through intracellular processes. For 13 of the 17 genes, this is the first report of a link to baz or the regulation of epithelial structure.
Highlights
Epithelial structure is essential for the development and homeostasis of multicellular organisms
We identified 17 genes that interact with Baz to regulate epithelial structure
For 13 of these, this is the first report of a role in epithelial polarity
Summary
Epithelial structure is essential for the development and homeostasis of multicellular organisms (for reviews see [1,2,3,4,5,6,7,8,9]). Each cell in an epithelial sheet has an apical domain facing the sheet surface and a basolateral domain facing underlying tissue. This polarity is tightly linked to epithelial structure. Microtubules (MTs) are organized in specific apical, lateral and basal networks, while intracellular trafficking pathways direct specific cargo to the apical or basolateral domains. This polarized organization of epithelial cells controls transport between body compartments, and is critical for the development and maintenance of epithelial structure. We sought to identify additional proteins that function with Baz to regulate epithelial structure in the Drosophila embryo
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