Expression of Inflammatory Modulator COX-2 in Pancreatic Ductal Adenocarcinoma and Its Relationship to Pathologic and Clinical Parameters

Merati, Kambiz; Siadaty, Mir S.; Andea, Aleodor A.; Sarkar, Fazlul H.; Ben‐Josef, Edgar; Mohammad, Ramzi M.; Philip, Philip; Shields, Anthony F.; Vaitkevicius, V. K.; Grignon, David J.; Adsay, Volkan

doi:10.1097/00000421-200110000-00007

Cited by 78 publications

(67 citation statements)

References 20 publications

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“…[3][4][5] Cox-2 overexpression leads to an enhanced production of prostaglandin E2 (PGE2), which is involved in tumor progression as well as in tumor evasion of immunosurveillance. 6 The release of PGE2 by cancer cells induces and recruits regulatory T cells to the tumor site and suppresses immune responses of CD8 C ab T cells and natural killer (NK) cells as well as maturation of dendritic cells.…”

Section: Introductionmentioning

confidence: 99%

Resistance of cyclooxygenase-2 expressing pancreatic ductal adenocarcinoma cells against γδ T cell cytotoxicity

Gonnermann

Oberg

Kellner³

et al. 2015

OncoImmunology

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Keywords: Cox-2, cytotoxicity, gammadelta T lymphocytes, human, pancreatic ductal adenocarcinoma, PGE2Abbreviations: BrHPP, bromohydrin-pyrophosphate; Cox, cyclooxygenase; n-BP, nitrogen-containing bisphosphonates; PAg, phosphorylated antigen; PDAC, pancreatic ductal adenocarcinoma; PG, prostaglandins; RTCA, Real Time Cell Analyzer; TCR, T cell receptor.The prostaglandin (PG) synthetase cyclooxygenase 2 (Cox-2) promotes tumorigenesis, tumor progression, and metastasis in a variety of human cancer entities including pancreatic ductal adenocarcinoma (PDAC). In this study, we demonstrate that in PDAC cells such as Colo357 cells, enhanced Cox-2 expression and increased release of the Cox-2 metabolite prostaglandin E2 (PGE2) promotes resistance against gd T cell-mediated lysis. Co-culture with activated gd T cells induced an upregulation of Cox-2 expression in Colo357 cells, and thereby an enhanced PGE2 release, in response to tumor necrosis factor a .TNFa/ secretion from gd T cells. The PGE2-mediated inhibition of gd T cell cytotoxicity against Cox-2-expressing PDAC cells can be partially overcome by Cox-2 inhibitors. Our results show that differences between PDAC cells in regards to sensitivity to gd T-cell cytotoxicity can be due to distinct levels of Cox-2 expression associated with varying amounts of PGE2 release. While gd T cell cytotoxicity against PDAC cells expressing low levels of Cox-2 can be effectively enhanced by tribody [(Her2) 2 £Vg9] with specificity for Vg9 T cell receptor and HER-2/neu on PDAC cells, a combination of tribody [(Her2) 2 £Vg9] and Cox-2 inhibitor is necessary to induce complete lysis of Cox-2 high expressing Colo357. In conclusion, our results suggest that the application of tribody [(Her2) 2 £Vg9] that enhances gd T-cell cytotoxicity and Cox-2 inhibitors that overcome PGE2-mediated resistance of PDAC cells to the cytotoxic activity of gd T cells might offer a promising combined immunotherapy for pancreatic cancer.

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Section: Introductionmentioning

confidence: 99%

Resistance of cyclooxygenase-2 expressing pancreatic ductal adenocarcinoma cells against γδ T cell cytotoxicity

Gonnermann

Oberg

Kellner³

et al. 2015

OncoImmunology

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“…[7][8][9][10][11] Increased expression of COX-2 has also been observed in pancreatic cancer, irrespective of histological type and grade, but the mechanisms that control the constitutive and induced expression of COX-2 in human pancreatic carcinoma cells are not completely understood. [12][13][14][15][16][17] The transcriptional activation of COX-2 is mediated by the binding of transcription factors to regulatory elements in the COX-2 promoters, such as nuclear factor κB (NF-κB), CCAAT/enhancerbinding protein (C/EBP), cyclic AMP response element-binding protein (CREB) and nuclear factor-activated T-cell/AP-1, which are involved in COX-2 induction in response to a variety of stimuli in different species and cell types. [18][19][20][21][22][23] For example, the C/EBP family of transcription factors plays an important role in COX-2 induction by lipopolysaccharide and phorbol ester in human vascular endothelial cells, 18 by tumor necrosis factor-α in murine MC3T3-E1 osteoblastic cells, 19 and in mouse skin carcinoma cells.…”

Section: Introductionmentioning

confidence: 99%

Prostaglandin E2 drives cyclooxygenase 2 expression via cyclic AMP response element activation in human pancreatic cancer cells

Pino

Nawrocki

Cognetti

et al. 2005

Cancer Biology & Therapy

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“…12 Mounting evidence derived from clinically proven biopsy samples showed that COX-2 is upregulated in human pancreatic tumor tissues as compared with normal adjacent pancreatic tissues. [13][14][15] Moreover, COX-2 inhibitors inhibit cell growth with greater efficacy in cell lines with stronger COX-2 expression compared with weakly COX-2 expressing PC cell lines. 14,16 Further studies have shown that genetic deletion of COX-2 abrogates tumorigenesis as well as intestinal polyposis in mouse model of familial adenomatous polyposis APC D716 compared with wild type animal.…”

mentioning

confidence: 99%

“…17,18 Studies from our laboratory have also shown over expression of COX-2 in pancreatic ductal adenocarcinoma, which was associated with increased perineural invasion. 15 Despite numerous advances in our understanding of the pathophysiology and molecular biology of PC, currently available standard therapeutic approach for PC show limited benefit in improving the survival of patients diagnosed with this deadly disease. NSAIDS are well studied class of chemopreventive agents and have been shown to act through both COX dependent 19,20 and independent pathways.…”

mentioning

confidence: 99%

A novel copper complex of 3‐benzoyl‐α methyl benzene acetic acid with antitumor activity mediated via cyclooxygenase pathway

Ahmed

Adsule

Ali

et al. 2006

Intl Journal of Cancer

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Pancreatic cancer (PC) is characterized as one of the deadliest malignancies and its treatment is a great challenge to clinical oncologists. Expression of COX-2 is detectable in 75% of PCs among which 50% showed overexpression, suggesting the importance of COX-2 enzyme and its metabolic product prostaglandin E2 (PGE 2 ) in PC. Here the authors report the synthesis and biological activity of a novel COX-2 inhibitor, FPA-306, and its effects on PC cells with different levels of COX-2 expression. Using MTT assay, the authors found a significant growth inhibition of BxPC-3 cells treated by FPA-306 with an IC 50 of 10 lmol/ L, which was lower than that of ketoprofen (IC 50 5 35.4 lmol/L) and celecoxib (IC 50 > 100 lmol/L). There was no such effect found in MIAPaCa cell line, which does not express COX-2. The authors also found dose dependent reduction in cell survival and induction of apoptosis by FPA-306 treatment in BxPC-3 cells but not in MIAPaCa cells. These results were correlated with apoptosis data and secreted PGE 2 levels. The molecular modeling of FPA-306 in the COX-2 active site showed that FPA-306 is potentially able to inhibit the activity of enzyme by blocking the active site, thereby resulting in decreased PGE 2 production. The authors also found a significant reduction of COX-2 at the mRNA and protein levels together with downregulation of NF-jB DNA binding activity and its downstream genes, Bcl-2 and survivin. These results suggest that FPA-306 is an effective and potent agent in inhibiting the growth of PC cells. ' 2006 Wiley-Liss, Inc.Key words: pancreatic cancer cells; cyclooxygenase-2; NSAIDS; prostaglandin E 2 Pancreatic cancer (PC) is the fourth leading cause of cancer related death in the United States. An estimated 33,730 individuals will be diagnosed with PC in the year of 2006, with an almost similar incidence rate among males and females. 1 PC is relatively resistant to all currently available therapeutic approaches including radiotherapy and chemotherapy. Palliative care is the only option because most of the patients are also not suitable for surgery at the time of diagnosis. Thus, delayed diagnosis partly due to indolent nature of pancreatic tumor progression and lack of effective therapy results in limited survival.From a mechanistic point of view, several molecular pathways have been identified such as Ras-Raf-MEK-ERK, PI3K/Akt and NF-jB pathway that are believed to be important in the development, progression and metastasis of PC. In addition, the involvement of cyclooxygenase (COX) and lipoxygenase family of enzymes in the development and progression of PC has been appreciated recently. 2 The COX family of enzymes catalyzes the ratelimiting step in conversion of arachidonic acid into prostaglandins. 3 Three isoforms of COX enzyme have been reported-COX-1, COX-2 and COX-3. 4 COX-1 is constitutively expressed in many tissues where it serves as house keeping gene whereas COX-2 is an inducible enzyme that is rapidly transcribed, perhaps regulated by NF-jB and other transcription factor...

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Expression of Inflammatory Modulator COX-2 in Pancreatic Ductal Adenocarcinoma and Its Relationship to Pathologic and Clinical Parameters

Cited by 78 publications

References 20 publications

Resistance of cyclooxygenase-2 expressing pancreatic ductal adenocarcinoma cells against γδ T cell cytotoxicity

Resistance of cyclooxygenase-2 expressing pancreatic ductal adenocarcinoma cells against γδ T cell cytotoxicity

Prostaglandin E2 drives cyclooxygenase 2 expression via cyclic AMP response element activation in human pancreatic cancer cells

A novel copper complex of 3‐benzoyl‐α methyl benzene acetic acid with antitumor activity mediated via cyclooxygenase pathway

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