AI Article Synopsis

  • The study focuses on membrane-bound mucins, specifically MUC3, MUC12, and MUC17, which are important for the gastrointestinal tract and are located on chromosome 7.
  • The researchers discovered that MUC17 has a strong interaction with PDZK1 and a weak interaction with NHERF1, while MUC12 shows weak binding to both PDZK1, NHERF1, and NHERF2.
  • Additionally, experiments indicated that PDZK1 stabilizes MUC3(17) in the apical membrane of small intestinal cells, as seen through differences in staining patterns in wild-type versus Pdzk1-/- mice.

Article Abstract

The membrane-bound mucins have a heavily O-glycosylated extracellular domain, a single-pass membrane domain and a short cytoplasmic tail. Three of the membrane-bound mucins,MUC3, MUC12 and MUC17, are clustered on chromosome 7 and found in the gastrointestinal tract. These mucins have C-terminal sequences typical of PDZ-domain-binding proteins. To identify PDZ proteins that are able to interact with the mucins,we screened PDZ domain arrays using YFP (yellow fluorescent protein)-tagged proteins. MUC17 exhibited a strong binding to PDZK1 (PDZ domain containing 1), whereas the binding toNHERF1 (Na+/H+-exchanger regulatory factor 1) was weak.Furthermore, we showed weak binding of MUC12 to PDZK1, NHERF1 and NHERF2. GST (glutathione transferase) pull-down experiments confirmed that the C-terminal tail of MUC17 coprecipitates with the scaffold protein PDZK1 as identified byMS. This was mediated through the C-terminal PDZ-interaction site in MUC17, which was capable of binding to three of the four PDZ domains in PDZK1. Immunostaining of wild-type or Pdzk1-/- mouse jejunum with an antiserum against Muc3(17),the mouse orthologue of human MUC17, revealed strong brushborder membrane staining in the wild-type mice compared with an intracellular Muc3(17) staining in the Pdzk1-/- mice. This suggests that Pdzk1 plays a specific role in stabilizing Muc3(17)in the apical membrane of small intestinal enterocytes.

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Source
http://dx.doi.org/10.1042/BJ20071068DOI Listing

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