Host Prostaglandin E2-EP3 Signaling Regulates Tumor-Associated Angiogenesis and Tumor Growth

Aoki, Hideki; Hayashi, Izumi; Endo, Hirahito; Kitasato, Hidero; Yamashina, Shohei; Maruyama, Takayuki; Kobayashi, M.; Satoh, Kazutoyo; Narita, Masami; Sugimoto, Yukihiko; Murata, Tatsunori; Yoshimura, Hirokuni; Narumiya, Shuh; Murakami, Masataka

doi:10.1084/jem.20021408

Cited by 303 publications

(242 citation statements)

References 50 publications

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“…This difference could be explained by the existence of multiple receptors on cell surfaces for PGE 2 , which could compensate or act instead of the EP2 receptor. In this context, it has been shown that human umbilical vein endothelial cells express both EP2 and EP4 (Dormond et al, 2002), and EP3-null mice show decreased tumor growth and angiogenesis (Amano et al, 2003). Moreover, deletion of EP1 and EP4 inhibits tumor development (Watanabe et al, 1999;Mutoh et al, 2002), clearly suggesting that different EP receptors may mediate specific aspects of tumor angiogenesis.…”

Section: Discussionmentioning

confidence: 99%

EP2, a receptor for PGE2, regulates tumor angiogenesis through direct effects on endothelial cell motility and survival

et al. 2006

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Prostaglandin E2 (PGE 2 ), a major cyclooxygenase (COX) metabolite, plays important roles in tumor biology. We studied the role of EP2, a receptor for PGE 2 , in tumor angiogenesis using EP2 knockout mice. We found that deletion of the EP2 receptor impaired tumor angiogenesis and this finding was confirmed by an in vivo corneal angiogenesis model and an ex vivo aortic ring assay. To further characterize the cellular mechanisms of the EP2 receptor in angiogenesis, we isolated primary pulmonary endothelial cells (ECs) from wild-type (wt) and EP2 À/À mice and observed that EP2 À/À ECs exhibited defects in vascular branch formation when compared to wt ECs. In addition, EP2 À/À ECs showed impaired cell motility on collagen-coated surface and they responded poorly to PGE 2 -induced cell migration compared to control cells. However, no difference in cell proliferation was observed between the EP2 À/À and wt Ecs. In addition, EP2 À/À ECs were more susceptible to apoptosis than wt cells under growth factor depletion conditions. Collectively, our data demonstrate that EP2 signaling in endothelium directly regulates tumor angiogenesis by contributing to cell survival and endothelial cell motility. Moreover, our finding suggests that EP2 is a major receptor in PGE 2 -mediated cell motility in ECs.

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Section: Discussionmentioning

confidence: 99%

EP2, a receptor for PGE2, regulates tumor angiogenesis through direct effects on endothelial cell motility and survival

et al. 2006

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“…12,13 However, little is known about the direct contribution of COX-2 to lymphedema-associated lymphangiogenesis, although positive correlations between COX-2 expression in tumor tissues and lymphangiogenesis and lymph node metastasis have been reported for several human cancers, [28][29][30] as well as the effect of COX-2 inhibition on lymphangiogenesis in a tumor implantation model. 14 In a study utilizing a nonselective COX inhibitor in a mouse tail lymphedema model, ketoprofen treatment normalized the histopathology with increased TNF-a expression and VEGF-C expression.…”

Section: Discussionmentioning

confidence: 99%

“…[10][11][12][13] In both inflammatory and tumor models, an inducible cyclooxygenase-2 (COX-2)-derived PGE 2 exerted proangiogenic activity via EP3 signaling, with the concomitant induction of VEGF-A. This effect was especially prominent in bone marrow (BM)-derived cells, which are a major component of tumor stromal tissues.…”

mentioning

confidence: 99%

Role of COX-2 in lymphangiogenesis and restoration of lymphatic flow in secondary lymphedema

Kashiwagi

Hosono

Suzuki

et al. 2011

Laboratory Investigation

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“…To this end, we used two selective EP 3 R antagonists L-798,106 [19] and ONO-AE 3 -240 [20]. As shown in Figure 4C and D, both EP 3 R antagonists (L-798,106 at 10 μM and ONO-AE 3 -240 at 10 nM) abolished the imetitinduced attenuation of NE exocytosis in cardiac synaptosomes.…”

Section: Increased Pge 2 Production Is Involved In the H 3 R-induced mentioning

confidence: 99%

Histamine H3-receptor signaling in cardiac sympathetic nerves: Identification of a novel MAPK-PLA2-COX-PGE2-EP3R pathway

Levi

Seyedi

Schäefer

et al. 2007

Biochemical Pharmacology

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We tested the hypothesis that the histamine H 3 -receptor (H 3 R)-mediated attenuation of norepinephrine (NE) exocytosis from cardiac sympathetic nerves results not only from a Gα imediated inhibition of the adenylyl cyclase-cAMP-PKA pathway, but also from a Gβγ i -mediated activation of the MAPK-PLA 2 cascade, culminating in formation of an arachidonate metabolite with anti-exocytotic characteristics (e.g., PGE 2 ). We report in Langendorff-perfused guinea-pig hearts and isolated sympathetic nerve endings (cardiac synaptosomes), H 3 R-mediated attenuation of K + -induced NE exocytosis was prevented by MAPK and PLA 2 inhibitors, and by cyclooxygenase and EP 3 -receptor (EP 3 R) antagonists. Moreover, H 3 R activation resulted in MAPK phosphorylation in H 3 R-transfected SH-SY5Y neuroblastoma cells, and in PLA 2 activation and PGE 2 production in cardiac synaptosomes; H 3 R-induced MAPK phosphorylation was prevented by an anti-βγ peptide. Synergism between H 3 R and EP 3 R agonists (i.e., imetit and sulprostone, respectively) suggested PGE 2 may be a downstream effector of the anti-exocytotic effect of H 3 R activation. Furthermore, the anti-exocytotic effect of imetit and sulprostone was potentiated by the N-type Ca 2+ -channel antagonist ω-conotoxin GVIA, and prevented by an anti-Gβγ peptide. Our findings suggest an EP 3 R Gβγ i -induced decrease in Ca 2+ influx through N-type Ca 2+ -channels is involved in PGE 2 / EP 3 R-mediated attenuation of NE exocytosis elicited by H 3 R activation. Conceivably, activation of the Gβγ i subunit of H 3 R and EP 3 R may also inhibit Ca 2+ entry directly, independent of MAPK intervention. As heart failure, myocardial ischemia and arrhythmic dysfunction are associated with excessive local NE release, attenuation of NE release by H 3 R activation is cardioprotective. Thus, the uncovering of a novel H 3 R signaling pathway may ultimately bear therapeutic significance in hyper-adrenergic states.

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Host Prostaglandin E2-EP3 Signaling Regulates Tumor-Associated Angiogenesis and Tumor Growth

Cited by 303 publications

References 50 publications

EP2, a receptor for PGE2, regulates tumor angiogenesis through direct effects on endothelial cell motility and survival

EP2, a receptor for PGE2, regulates tumor angiogenesis through direct effects on endothelial cell motility and survival

Role of COX-2 in lymphangiogenesis and restoration of lymphatic flow in secondary lymphedema

Histamine H3-receptor signaling in cardiac sympathetic nerves: Identification of a novel MAPK-PLA2-COX-PGE2-EP3R pathway

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