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Claudins and JAM-A coordinately regulate tight junction formation and epithelial polarity. | LitMetric

AI Article Synopsis

  • Tight junctions (TJs) are crucial for maintaining the epithelial barrier and regulating cell polarity, though their exact role remains debated.
  • Claudins and cytoplasmic proteins ZO-1 and ZO-2 are key components of TJs, with ZO proteins essential for TJ structure and epithelial barrier function while claudins contribute to electrolyte permeability.
  • The study found that claudins help form membrane connections and maintain macromolecule permeability, while ZO-deficient cells showed disorganized polarity, indicating that claudins and JAM-A work together to coordinate TJ formation and epithelial cell orientation.

Article Abstract

Tight junctions (TJs) establish the epithelial barrier and are thought to form a membrane fence to regulate epithelial polarity, although the roles of TJs in epithelial polarity remain controversial. Claudins constitute TJ strands in conjunction with the cytoplasmic scaffolds ZO-1 and ZO-2 and play pivotal roles in epithelial barrier formation. However, how claudins and other TJ membrane proteins cooperate to organize TJs remains unclear. Here, we systematically knocked out TJ components by genome editing and show that while ZO-1/ZO-2-deficient cells lacked TJ structures and epithelial barriers, claudin-deficient cells lacked TJ strands and an electrolyte permeability barrier but formed membrane appositions and a macromolecule permeability barrier. Moreover, epithelial polarity was disorganized in ZO-1/ZO-2-deficient cells, but not in claudin-deficient cells. Simultaneous deletion of claudins and a TJ membrane protein JAM-A resulted in a loss of membrane appositions and a macromolecule permeability barrier and in sporadic epithelial polarity defects. These results demonstrate that claudins and JAM-A coordinately regulate TJ formation and epithelial polarity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6781433PMC
http://dx.doi.org/10.1083/jcb.201812157DOI Listing

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