AI Article Synopsis

  • MUPP1 and Patj are proteins found in tight junctions of epithelial cells, both featuring L27 and PDZ domains but differing in number (MUPP1 has 13 PDZ domains; Patj has 10).
  • While Patj is essential for establishing tight junctions and epithelial polarity, MUPP1 does not play a critical role in these processes, despite sharing binding partners and localization mechanisms with Patj.
  • Research indicates that Pals1, which preferentially binds to Patj, is crucial for activating the Par6-aPKC complex, highlighting the functional differences between MUPP1 and Patj in epithelial cells.

Article Abstract

MUPP1 and Patj are both composed of an L27 domain and multiple PDZ domains (13 and 10 domains, respectively) and are localized to tight junctions (TJs) in epithelial cells. Although Patj is known to be responsible for the organization of TJs and epithelial polarity, characterization of MUPP1 is lacking. In this study, we found that MUPP1 and Patj share several binding partners, including JAM1, ZO-3, Pals1, Par6, and nectins (cell-cell adhesion molecules at adherens junctions). MUPP1 and Patj exhibited similar subcellular distributions, and the mechanisms with which they localize to TJs also appear to overlap. Despite these similarities, functional studies have revealed that Patj is indispensable for the establishment of TJs and epithelial polarization, whereas MUPP1 is not. Thus, although MUPP1 and Patj share several molecular properties, their functions are entirely different. We present evidence that the signaling mediated by Pals1, which has a higher affinity for Patj than for MUPP1 and is involved in the activation of the Par6-aPKC complex, is of principal importance for the function of Patj in epithelial cells.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2668367PMC
http://dx.doi.org/10.1128/MCB.01505-08DOI Listing

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