3.9 Article

Adaptor protein 1 B mu subunit does not contribute to the recycling of kAE1 protein in polarized renal epithelial cells

期刊

MOLECULAR MEMBRANE BIOLOGY
卷 34, 期 1-2, 页码 50-64

出版社

TAYLOR & FRANCIS LTD
DOI: 10.1080/09687688.2018.1451662

关键词

Kidney; adaptor proteins; membrane protein; epithelium; trafficking; endocytosis; recycling; distal renal tubular acidosis

资金

  1. Kidney Foundation of Canada [KFOC140013, KFOC170007]
  2. Canadian Institutes of Health Research
  3. Canada Foundation for Innovation
  4. NSERC CREATE Team grant in Membrane Biology
  5. Women and Children's Health Research Institute
  6. KRESCENT New Investigator

向作者/读者索取更多资源

Mutations in the gene encoding the kidney anion exchanger 1 (kAE1) can lead to distal renal tubular acidosis (dRTA). dRTA mutations reported within the carboxyl (C)-terminal tail of kAE1 result in apical mis-targeting of the exchanger in polarized renal epithelial cells. As kAE1 physically interacts with the subunit of epithelial adaptor protein 1 B (AP-1B), we investigated the role of heterologously expressed 1B subunit of the AP-1B complex for kAE1 retention to the basolateral membrane in polarized porcine LLC-PK1 renal epithelial cells that are devoid of endogenous AP-1B. We confirmed the interaction and close proximity between kAE1 and 1B using immunoprecipitation and proximity ligation assay, respectively. Expressing the human 1B subunit in these cells decreased significantly the amount of cell surface kAE1 at the steady state, but had no significant effect on kAE1 recycling and endocytosis. We show that (i) heterologous expression of 1B displaces the physical interaction of endogenous GAPDH with kAE1WT supporting that both AP-1B and GAPDH proteins bind to an overlapping site on kAE1 and (ii) phosphorylation of tyrosine 904 within the potential YDEV interaction motif does not alter the kAE1/AP-1B interaction. We conclude that 1B subunit is not involved in recycling of kAE1.

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