Prostaglandin E<sub>2</sub> upregulates EGF‐stimulated signaling in mitogenic pathways involving Akt and ERK in hepatocytes

Dajani, Olav; Meisdalen, Kristin; Guren, Tormod Kyrre; Aasrum, Monica; Tveteraas, Ingun Heiene; Lilleby, Peggy; Thoresen, G. Hege; Sandnes, Dagny; Christoffersen, Thoralf

doi:10.1002/jcp.21205

Cited by 46 publications

(45 citation statements)

References 77 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…This is in agreement with our previous observation that cAMP does not mediate the proliferative effects of prostaglandins in the hepatocytes (Refsnes et al, 1995). Furthermore, although EP4 receptors have been found to stimulate cyclin D1 expression and phosphorylation of EGF receptor and extracellular signal-regulated kinase in murine hepatocytes (Kataoka et al, 2005), prostaglandins do not transactivate the EGF receptor in rat hepatocytes (Nilssen et al, 2004) but act to enhance subsequent stimulation of extracellular signal-regulated kinase and Akt by EGF (Dajani et al, 2007). In addition, we found no additive effects between sulprostone and misoprostol on DNA synthesis, suggesting lack of involvement of EP4 receptors.…”

Section: Discussionsupporting

confidence: 93%

Prostaglandins Enhance Epidermal Growth Factor-Induced DNA Synthesis in Hepatocytes by Stimulation of E Prostanoid 3 and F Prostanoid Receptors

Meisdalen

Dajani²,

Christoffersen³

et al. 2007

J Pharmacol Exp Ther

Self Cite

View full text Add to dashboard Cite

Prostaglandins stimulate hepatocyte proliferation in vivo and in vitro. We have examined the role of E prostanoid (EP) and F prostanoid receptors (FP) in enhancing the growth-stimulatory effect of epidermal growth factor (EGF) in cultured hepatocytes. The EP2 receptor agonist butaprost had no significant effect on EGF-induced DNA synthesis. EP1 receptor-selective antagonists did not affect the enhancement by prostaglandin E 2 of EGF-stimulated DNA synthesis. Sulprostone, misoprostol, and fluprostenol strongly enhanced DNA synthesis and inhibited glucagon-stimulated cAMP accumulation, indicating that they all activated EP3 receptors. Combining fluprostenol with misoprostol, but not with sulprostone, resulted in partially additive effects on DNA synthesis, suggesting that both EP3 and FP receptors are involved. Combining sulprostone with misoprostol did not result in additive effects on DNA synthesis, suggesting that EP4 receptors were not involved. We conclude that, although a minor effect is exerted by FP receptors, the growth-stimulatory effects of prostaglandins in rat hepatocytes are mediated mainly by EP3 receptors. We have found no evidence of EP1 receptor involvement.

show abstract

Section: Discussionsupporting

confidence: 93%

Prostaglandins Enhance Epidermal Growth Factor-Induced DNA Synthesis in Hepatocytes by Stimulation of E Prostanoid 3 and F Prostanoid Receptors

Meisdalen

Dajani²,

Christoffersen³

et al. 2007

J Pharmacol Exp Ther

Self Cite

View full text Add to dashboard Cite

show abstract

“…EGFR is a multifunctional tyrosine kinase receptor with the ability to active multiple effectors and downstream signaling pathways (48,49). In the current study, we observed that EP2 agonist-mediated transactivation of EGFR resulted in the activation of the downstream signaling effectors: ERK1/2, Akt, and STAT3.…”

Section: Discussionmentioning

confidence: 54%

“…ERK1/2 and Akt are known to be activated in cultured cells by PGE 2 (20,48,50) and to play important roles in cell proliferation and skin tumor formation (33,36). Several reports indicated that PGE 2 -stimulated ERK1/2 and Akt activation were mediated by both activated EGFR and activated PKA (20,48,51) and that both effectors contributed to keratinocyte replication and survival (33,35). However, in the present studies, Akt activation was suppressed by EGFR inhibition but not by inhibition of PKA (Figs.…”

Section: Discussionmentioning

confidence: 99%

The Prostaglandin E2 Receptor, EP2, Stimulates Keratinocyte Proliferation in Mouse Skin by G Protein-dependent and β-Arrestin1-dependent Signaling Pathways

Chun

Lao

Langenbach

2010

Journal of Biological Chemistry

View full text Add to dashboard Cite

Because keratinocyte proliferation is essential for skin tumor development, EP2-mediated signaling pathways that contribute to keratinocyte proliferation were investigated. A single topical application of the EP2 agonist, butaprost, dose-dependently increased keratinocyte replication via activation of epidermal growth factor receptor (EGFR) and PKA signaling. Because GPCR-mediated activation of EGFR can involve the formation of a GPCR-␤-arrestin-Src signaling complex, the possibility of a ␤-arrestin1-Src complex contributing to EP2-mediated signaling in keratinocytes was investigated. Butaprost induced ␤-arrestin1-Src complex formation and increased both Src and EGFR activation. A role for ␤-arrestin1 in EP2-mediated Src and EGFR activation was demonstrated by the observation that ␤-arrestin1 deficiency significantly reduced Src and EGFR activation. In agreement with a ␤-arrestin1-Src complex contributing to EGFR activation, Src and EGFR inhibition (PP2 and AG1478, respectively) indicated that Src was upstream of EGFR. Butaprost also induced the activation of Akt, ERK1/2, and STAT3, and both ␤-arrestin1 deficiency and EGFR inhibition (AG1478 or gefitinib) decreased their activation. In addition to ␤-arrestin1-dependent EGFR activation, butaprost increased PKA activation, as measured by phospho-GSK3␤ (p-GSK3␤) and p-cAMP-response element-binding protein formation. PKA inhibition (H89 or R P -adenosine-3,5-cyclic monophosphorothioate (R P -cAMPS)) decreased butaprost-induced cAMP-response element-binding protein and ERK activation but did not affect EGFR activation, whereas ␤-arrestin1 deficiency decreased EGFR activation but did not affect butaprost-induced PKA activation, thus indicating that they were independent EP2-mediated pathways. Therefore, the results indicate that EP2 contributed to mouse keratinocyte proliferation by G protein-independent, ␤-arrestin1-dependent activation of EGFR and G protein-dependent activation of PKA.

show abstract

“…From a more generalized view, prostaglandins may act to potentiate the action of growth factor signals. In an analogous model, PGE 2 may augment the action of platelet-derived growth factor; PGE 2 has low mitotic activity on its own but augments the platelet-derived growth factor signal to increase cell growth (11). Thus, some prostaglandins may act to modulate trophic signals, providing another level of regulation for key signaling pathways.…”

Section: Discussionmentioning

confidence: 99%

Targeting steroid receptor coactivator 1 with antisense oligonucleotides increases insulin-stimulated skeletal muscle glucose uptake in chow-fed and high-fat-fed male rats

Cantley

Vatner²,

Galbo³

et al. 2014

American Journal of Physiology-Endocrinology and Metabolism

View full text Add to dashboard Cite

Ϫ/Ϫ mice have decreased hepatic expression of gluconeogenic enzymes and a reduction in the rate of endogenous glucose production (EGP). We sought to determine whether decreasing hepatic and adipose SRC1 expression in normal adult rats would alter glucose homeostasis and insulin action. Regular chow-fed and high-fat-fed male Sprage-Dawley rats were treated with an antisense oligonucleotide (ASO) against SRC1 or a control ASO for 4 wk, followed by metabolic assessments. SRC1 ASO did not alter basal EGP or expression of gluconeogenic enzymes. Instead, SRC1 ASO increased insulin-stimulated whole body glucose disposal by ϳ30%, which was attributable largely to an increase in insulinstimulated muscle glucose uptake. This was associated with an approximately sevenfold increase in adipose expression of lipocalintype prostaglandin D 2 synthase, a previously reported regulator of insulin sensitivity, and an approximately 70% increase in plasma PGD 2 concentration. Muscle insulin signaling, AMPK activation, and tissue perfusion were unchanged. Although GLUT4 content was unchanged, SRC1 ASO increased the cleavage of tether-containing UBX domain for GLUT4, a regulator of GLUT4 translocation. These studies point to a novel role of adipose SRC1 as a regulator of insulin-stimulated muscle glucose uptake. insulin resistance; glucose transporter type 4; skeletal muscle; white adipose tissue GLUCOSE HOMEOSTASIS REQUIRES THE COMPLEX COORDINATION of cellular and molecular pathways in multiple tissues. In many instances, these pathways collate hormonal and metabolic cues to regulate transcription factors that alter the expression of genes encoding key metabolic enzymes. The activity of transcription factors is regulated further by transcriptional coactivators and corepressors. The three members of the p160 steroid coactivator receptor family, the steroid receptor coactivator 1 (SRC1 or NcoA-1), the transcriptional intermediary factor 2 (TIF2, SRC2, GRIP1, or NCOA2), and steroid receptor coactivator 3 (SRC3, p/CIP, AIB1, ACTR, RAC3, or TRAM-1) have all been shown to control energy balance through their interactions with many transcription factors, including nuclear receptors (14,16,18,22). The SRC1 family has also been implicated in many other physiological processes, including reproduction, cancer, and immunity (22,27,42,49,50).A significant body of work has shown that SRC1 is important for the tissue-specific activation of progesterone and estrogen receptors (1,16,42). Additionally, studies using the SRC1 global knockout mice have shown that SRC1 is required for uterine growth and function, prostate development, mammary gland growth and elongation, brain development and function, and metabolism (20,23,24,28,31,49,50,52). SRC1 Ϫ/Ϫ mice also have features of thyroid hormone resistance, with evidence that SRC1 is critical for proper activation of the thyroid hormone receptor-␤ (48). SRC1 Ϫ/Ϫ mice have impairment in brown adipose tissue (BAT) function that makes them prone to weight gain potentially through decreased activation of PGC-1...

show abstract

Prostaglandin E₂ upregulates EGF‐stimulated signaling in mitogenic pathways involving Akt and ERK in hepatocytes

Cited by 46 publications

References 77 publications

Prostaglandins Enhance Epidermal Growth Factor-Induced DNA Synthesis in Hepatocytes by Stimulation of E Prostanoid 3 and F Prostanoid Receptors

Prostaglandins Enhance Epidermal Growth Factor-Induced DNA Synthesis in Hepatocytes by Stimulation of E Prostanoid 3 and F Prostanoid Receptors

The Prostaglandin E2 Receptor, EP2, Stimulates Keratinocyte Proliferation in Mouse Skin by G Protein-dependent and β-Arrestin1-dependent Signaling Pathways

Targeting steroid receptor coactivator 1 with antisense oligonucleotides increases insulin-stimulated skeletal muscle glucose uptake in chow-fed and high-fat-fed male rats

Contact Info

Product

Resources

About

Prostaglandin E2 upregulates EGF‐stimulated signaling in mitogenic pathways involving Akt and ERK in hepatocytes

Cited by 46 publications

References 77 publications

Prostaglandins Enhance Epidermal Growth Factor-Induced DNA Synthesis in Hepatocytes by Stimulation of E Prostanoid 3 and F Prostanoid Receptors

Prostaglandins Enhance Epidermal Growth Factor-Induced DNA Synthesis in Hepatocytes by Stimulation of E Prostanoid 3 and F Prostanoid Receptors

The Prostaglandin E2 Receptor, EP2, Stimulates Keratinocyte Proliferation in Mouse Skin by G Protein-dependent and β-Arrestin1-dependent Signaling Pathways

Targeting steroid receptor coactivator 1 with antisense oligonucleotides increases insulin-stimulated skeletal muscle glucose uptake in chow-fed and high-fat-fed male rats

Contact Info

Product

Resources

About

Prostaglandin E₂ upregulates EGF‐stimulated signaling in mitogenic pathways involving Akt and ERK in hepatocytes