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Polarized epithelia, such as hepatocytes, target their integral membrane proteins to specific apical or basolateral membrane domains during or after biogenesis. The roles played by protein glycosylation in this sorting process remain controversial. We report here that deglycosylation treatments in well-polarized hepatic cells by deglycosylation drugs, or by site-directed mutagenesis of the N-linked-glycosylation residues, all cause the Na+/K+-ATPase
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JCS ePress
online publication date 8 Dec 2005
doi: 10.1242/jcs.02706
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Research Article
Deglycosylation of Na+/K+-ATPase causes the basolateral protein to undergo apical targeting in polarized hepatic cells
* Author for correspondence (e-mail: linch{at}ym.edu.tw)
-subunit to traffic from the native basolateral to the apical/canalicular domain. Deglycosylated
-subunits are still able to bind and therefore transport the catalytic
-subunits to the aberrant apical location. Such apical targeting is mediated via the indirect transcytosis pathway. Cells containing apical Na+/K+-ATPase appear to be defective in maintaining the ionic gradient across the plasma membrane and in executing hepatic activities that are dependent upon the ionic homeostasis such as canalicular excretion.![]()
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Y.-H. Yi, P.-Y. Ho, T.-W. Chen, W.-J. Lin, V. Gukassyan, T.-H. Tsai, D.-W. Wang, T.-S. Lew, C.-Y. Tang, S. J. Lo, et al.
Membrane Targeting and Coupling of NHE1-Integrin{alpha}IIb{beta}3-NCX1 by Lipid Rafts following Integrin-Ligand Interactions Trigger Ca2+ Oscillations
J. Biol. Chem.,
February 6, 2009;
284(6):
3855 - 3864.
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