4.6 Article

Phospholipase C-γ Binds Directly to the Na+/H+ Exchanger 3 and Is Required for Calcium Regulation of Exchange Activity

期刊

JOURNAL OF BIOLOGICAL CHEMISTRY
卷 284, 期 29, 页码 19437-19444

出版社

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M109.006098

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资金

  1. National Institutes of Health Grants [R01-DK26523, R01-DK61765, PO1-DK72084, R24-DK64388]
  2. The Hopkins Center for Epithelial Disorders Grants [T32-DK07632, K01-DK080930]
  3. Searle Young Investigators award
  4. Pennsylvania State University
  5. Huck Life Science Institute Center for Computational Proteomics
  6. Pennsylvania Department of Health using Tobacco Settlement Funds
  7. Direct For Biological Sciences
  8. Div Of Molecular and Cellular Bioscience [0843282] Funding Source: National Science Foundation

向作者/读者索取更多资源

Multiple studies suggest that phospholipase C-gamma(PLC-gamma) contributes to regulation of sodium/hydrogen exchanger 3 (NHE3) in the small intestine, although the mechanism(s) for this regulation remain unknown. We demonstrate here that PLC-gamma binds directly to the C terminus of NHE3 and exists in similar sized multiprotein complexes as NHE3. This binding is dynamic and decreases with elevated [Ca2+](i). The PLC-gamma-binding site in NHE3 was identified (amino acids 586-605) and shown to be a critical regulatory domain for protein complex formation, because when it is mutated, NHE3 binding to PLC-gamma as well as NHERF2 is lost. An inhibitory peptide, which binds to the Src homology 2 domains contained in PLC-gamma without interrupting binding of PLC-gamma to NHE3, was used to probe a non-lipase-dependent role of PLC-gamma. In the presence of this peptide, carbachol-stimulated calcium inhibition of NHE3 was lost. These results mirror previous studies with the transient receptor potential channel and suggest that PLC-gamma may play a common role in regulating the cell-surface expression of ion transporters.

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