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JBC, Vol. 252, Issue 9, 2900-2907, May, 1977
J. H. Heaton and T. D. Gelehrter
Amino acid starvation causes an adaptive increase in the initial rate of
transport of selected neutral amino acids in an established line of rat
hepatoma cells in tissue culture. After a lag of 30 min, the initial rate
of transport of alpha-aminoisobutyric acid (AIB) increases to a maximum
after 4 to 6 h starvation of 2 to 3 times that seen in control cells. The
increased rate of transport is accompanied by an increase in the Vmax and a
modest decrease in the Km for this transport system, and is reversed by
readdition of amino acids. The enhancement is specific for amino acids
transported by the A or alanine-preferring system (AIB, glycine, proline);
uptake of amino acids transported by the L or leucine-preferring system
(threonine, phenylalanine, tyrosine, leucine) or the Ly+ system for dibasci
amino acids (lysine) is decreased under these conditions. Amino acids which
compete with AIB for transport also prevent the starvation-induced increase
in AIB transport; amino acids which do not compete fail to prevent the
enhancement. Paradoxically threonine, phenylalanine, tryptophan, and
tyrosine, which do not compete with AIB for transport, block the
enhancement of transport upon amino acid starvation. The starvation-induced
enhancement of amino acid transport does not appear to be the result of a
release from transinhibition. After 30 min of amino acid starvation, AIB
transport is either unchanged or slightly decreased even though amino acid
pools are already depleted. Furthermore, loading cells with high
concentrations of a single amino acid following a period of amino acid
starvation fails to prevent the enhancement of AIB transport, whereas
incubation of the cells with the single amino acid for the entire duration
of amino acid starvation prevents the enhancement; intracellular amino acid
pools are similar under both conditions. The enhancement of amino acid
transport requires concomitant RNA and protein synthesis, consistent with
the view that the adaptive increase reflects an increased amount of a
rate-limiting protein involved in the transport process. Dexamethasone,
which dramatically inhibits AIB transport in cells incubated in amino
acid-containing medium, both blocks the starvation-induced increase in AIB
transport, and causes a time-dependent decrease in transport velocity in
cells whose transport has previously been enhanced by starvation.
Derepression of amino acid transport by amino acid starvation in rat hepatoma cells
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