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Neutral amino acid transport in human synovial cells: Substrate specificity of adaptative regulation and transinhibition

✍ Scribed by Christian Aussel; Sophie Rousseau-Loric; Luc Cynober; Jean Agneray; Ohvanesse G. Ekindjian

Publisher: John Wiley and Sons
Year: 1989
Tongue: English
Weight: 769 KB
Volume: 141
Category: Article
ISSN: 0021-9541
DOI: 10.1002/jcp.1041410116

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✦ Synopsis

Neutral amino acid transport was characterired in human synovial cells. The amino acids tested are transported by all three major neutral amino acid transport systems, that is, A, L, and ASC. The model amino acid 2-aminoisobutyric acid (AIB) was found to be a strong specific substrate for system A in synovial cells. When cells were starved of amino acids, the activity of AIB transport increased, reaching a maximum within 1 h. The stimulation of transport activity was not blocked by cycloheximide and would thus appear to be related to a release from transinhibition. Similarly, the decrease in the activity of AIB transport observed after the addition of a-methyl-aminoisobutyric acid (meAIB) appeared to be related to transinhibition. However, using a different approach, that is, amino acid starvation followed by incubation with 10 mM meAlB and transfer to an amino acid-free medium with or without cycloheximide supplementation, a clear increase in AIB uptake, due both to derepression and a release from transinhibition, was observed. Unlike human fibroblasts, the derepression of system A in these synovial cells was not serum-dependent. The process of derepression was observed only after preloading with meAIB. Neither AIB nor alanine produced this phenomenon. Moreover, alanine preloading led to a large increase in AIB transport activity due to a release from transinhibition. These observations indicate that the process of derepression and release from transinhibition are specific to the substrates present in the culture medium prior to amino acid starvation.

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