TABLE 2.
EFFECT OF LPS ON GSH, CySS, CyS TRANSPORT (SYSTEMS)
| Thiol/Transport System | Effects | Model | Mechanism | Putative Function | Ref. |
|---|---|---|---|---|---|
| GSH/transporter unknown | 300% increase in GSH efflux, 15 min after LPS* (5 mg/kg body wt; intravenously) | In vivo, hepatic sinusoids | Increase activity of GSH transporter by LPS-mediated induction of complement | Protect against extracellular oxidant stress | (9) |
| Cystine/xc− | ∼3-fold increase in CySS influx, 6 h after LPS (1 ng/ml) | In vitro, murine primary peritoneal macrophages | Transcriptional upregulation of xCT | Increase cellular GSH | (37) |
| Cysteine/A, ASC | ∼2.7-fold increase in Cys influx 4 h after LPS (7.5mg/kg body wt; intraperitoneally) | Ex vivo, hepatic membrane vesicles | Increase in Vmax of System A and ASC by LPS-mediated induction of cortisol, TNF-α, and cyclooxygenase- derived products | Support gluconeogenesis and synthesis of acute phase proteins | (41) |
Definition of abbreviations: ASC, Na+-dependent neutral amino acid transporter; CyS, cysteine; CySS, disulfide cysteine; GSH, glutathione; xCT, subunit of the CySS transporter.
*
Salmonella enteritidis LPS.