Cytokines, endotoxin, and glucocorticoids regulate the expression of inducible nitric oxide synthase in hepatocytes.

Abstract: Nitric oxide (NO-) is a short-lived mediator which can be induced in a variety of cell types and produces many physiologic and metabolic changes in target cells. The inducible or high-output NO' synthase (NOS) pathway was first characterized in macrophages activated by lipopolysaccharide (LPS) and interferon v (IFN-y). Hepatocytes also express an inducible NOS following exposure to the combination of endotoxin (LPS) and tumor necrosis factor (TNF), interleukin 1 Following the discovery of the nitric oxide (NO-… Show more

“…We previously showed that DEX inhibits inducible nitric oxide synthase gene expression and nitric oxide production in cultured primary hepatocytes stimulated with TNF-a and interleukin-1b by suppressing NF-kB activation. 34,35 Furthermore, DEX can inhibit the production of proinflammatory cytokines in immune cells by the suppression of NF-kB activation. 5 We found that pretreatment of hepatocytes with DEX for 2-12 h inhibited NF-kB activation, as determined by gel-shift assay, in cultured rat primary hepatocytes stimulated with TNF-a (data not shown), suggesting that DEX-mediated upregulation of cFLIP is not due to NF-kB activation.…”

Dexamethasone protects primary cultured hepatocytes from death receptor-mediated apoptosis by upregulation of cFLIP

“…We previously showed that DEX inhibits inducible nitric oxide synthase gene expression and nitric oxide production in cultured primary hepatocytes stimulated with TNF-a and interleukin-1b by suppressing NF-kB activation. 34,35 Furthermore, DEX can inhibit the production of proinflammatory cytokines in immune cells by the suppression of NF-kB activation. 5 We found that pretreatment of hepatocytes with DEX for 2-12 h inhibited NF-kB activation, as determined by gel-shift assay, in cultured rat primary hepatocytes stimulated with TNF-a (data not shown), suggesting that DEX-mediated upregulation of cFLIP is not due to NF-kB activation.…”

Dexamethasone protects primary cultured hepatocytes from death receptor-mediated apoptosis by upregulation of cFLIP

“…NO production by inducible NOS (iNOS) in the liver, in contradistinction to eNOS generation of NO, is independent of calcium and largely dependent on the level of iNOS gene expression. 41 Although the liver is not thought to express iNOS basally, every major cell type in the liver expresses iNOS under appropriate circumstances, particularly the hepatocyte. 42 TNF-␣, interleukin 1␤, and interferon gamma all have the capability to induce iNOS transcription in hepatocytes, although IL-1 is the most potent in human and rat hepatocytes.…”

The hepatic circulation in health and disease: Report of a single-topic symposium

“…In vitro, interleukin-1 (IL-1), tumor necrosis factor (TNF), interferon-γ (IFN-γ), and bacterial lipopolysaccharide (LPS) act synergistically to induce iNOS expression maximally in hepatocytes. [15] Interleukin-1 is the most potent single inducer of iNOS, [16] while redox stress further activates iNOS gene transcription. [11] In vivo, hepatocyte iNOS expression has been identified in response to endotoxemia, [17] hemorrhagic shock, [18,19] hepatic and intestinal ischemia/reperfusion, [20] and during hepatic regeneration [21] or hepatitis.…”

Inflammatory Modulation of Hepatocyte Apoptosis by Nitric Oxide: In Vivo, In Vitro, and In Silico Studies