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J. Biol. Chem., Vol. 263, Issue 27, 13683-13691, 09, 1988
AN Yusufi, M Szczepanska-Konkel and TP Dousa
The role of N-linked oligosaccharide side chains in the biogenesis and
function of Na+-coupled transporters in renal luminal brush-border membrane
(BBM) is not known. We examined the question of how in vivo inhibition by
alkaloid swainsonine of alpha-mannosidase, a key enzyme in processing of
glycoproteins in the Golgi apparatus, affects Na+/H+ antiport and Na+/Pi
symport as well as activities of other transporters and enzymes in rat
renal BBM. Administration of swainsonine to thyroparathyroidectomized rats,
control or treated with 3,5,3'- triiodothyronine, markedly decreased the
rate of Na+/H+ antiport, but had no effect on the rate of Na+/Pi symport
across renal BBM vesicles (BBMV). Moreover, administration of swainsonine
did not change activities of Na+ gradient, ([extravesicular Na+] greater
than [intravesicular Na+])-dependent transport of D-glucose, L-proline, or
the amiloride-insensitive 22Na+ uptake by BBMV; the activities of the BBM
enzymes alkaline phosphatase, gamma-glutamyltransferase, or leucine
aminopeptidase in BBMV were also not changed. The in vitro enzymatic
deglycosylation of BBM by incubating freshly isolated BBMV with bacterial
endoglycosidase F also resulted in a decreased rate of Na+/H+ antiport, but
not Na+-coupled symports of Pi, L-proline, and D-glucose, or the activities
of the BBM enzymes were not significantly affected. Similar incubation with
endoglycosidase H was without effect on any of these parameters. Both the
modification of BBMV glycoproteins by administration fo swainsonine in vivo
as well as the in vitro incubation of BBMV with endoglycosidase F resulted
in a decrease of the apparent Vmax of Na+/H+ antiport, but did not change
the apparent Km of this antiporter for extravesicular Na+ and did not
increase H+ conductance of BBM. Taken together, our findings suggest that
intact N- linked oligosaccharide chains of the biantennary complex type in
renal BBM glycoproteins are required, directly or indirectly, for the
transport function of the Na+/H+ antiporter inserted into BBM of renal
proximal tubules.
Role of N-linked oligosaccharides in the transport activity of the Na+/H+ antiporter in rat renal brush-border membrane
Department of Physiology and Biophysics, Mayo Clinic and Foundation, Mayo Medical School, Rochester, Minnesota 55905.
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