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J. Biol. Chem., Vol. 265, Issue 24, 14321-14326, 08, 1990
ME Mailliard and MS Kilberg
The activities of several selected Na(+)-dependent amino acid transporters
were identified in human liver plasma membrane vesicles by testing for
Na(+)-dependent uptake of several naturally occurring neutral amino acids
or their analogs. Alanine, 2- (methylamino)isobutyric acid, and
2-aminoisobutyric acid were shown to be almost exclusively transported by
the same carrier, system A. Kinetic analysis of 2-(methylamino)isobutyric
acid uptake by the human hepatic system A transporter revealed an apparent
Km of 0.15 mM and a Vmax of 540 pmol.mg-1 protein.min-1. Human hepatic
system A accepts a broad range of neutral amino acids including cysteine,
glutamine, and histidine, which have been shown in other species to be
transported mainly by disparate carriers. Inhibition analysis of
Na(+)-dependent cysteine transport revealed that the portion of uptake not
mediated by system A included at least two saturable carriers, system ASC
and one other that has yet to be characterized. Most of the glutamine and
histidine uptake was Na(+)-dependent, and the component not mediated by
system A constituted system N. The largest portion of glycine transport was
mediated through system A and the remainder by system ASC with no evidence
for system Gly activity. Our examination of Na(+)-dependent amino acid
transport documents the presence of several transport systems analogous to
those described previously but with some notable differences in their
functional activity. Most importantly, the results demonstrate that liver
plasma membrane vesicles are a valuable resource for transport analysis of
human tissue.
Sodium-dependent neutral amino acid transport by human liver plasma membrane vesicles
Department of Medicine, University of Florida College of Medicine, Gainesville 32610.
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