The role of prostacyclin synthase and thromboxane synthase signaling in the development and progression of cancer

Cathcart, Mary-Clare; Reynolds, John V.; O’Byrne, Kenneth J.; Pidgeon, Graham P.

doi:10.1016/j.bbcan.2010.01.006

Cited by 48 publications

(61 citation statements)

References 173 publications

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“…to an increase in apoptosis regardless of cell type, which is supported by the previous reports showing that inhibition of TxAS resulted in apoptosis in bladder (Moussa et al, 2008a) and lung (Cathcart et al, 2010) cancer cells, and that treatment with TxA 2 receptor antagonists also caused significant apoptosis in bladder cancer cells (Moussa et al, 2008b).…”

Section: Discussionsupporting

confidence: 83%

“…In addition, the bladder cancer cells transfected with b-isoform of TxA 2 receptor and stimulated with U46619 resulted in a significant increase in cellular growth rate and PCNA expression (Moussa et al, 2008b). A recent study has also reported that treatment of two NSCLC cell lines with another selective TxAS inhibitor ozagrel induced a significant reduction in cell proliferation (Cathcart et al, 2010). We have further demonstrated that the inhibitory effect of furegrelate or SQ29548 on NNK-promoted cell proliferation/survival is in part due Figure 5 Effects of blocking TxA 2 synthesis and action on Akt, ERK, JNK and p38 in cells exposed to NNK.…”

Section: Discussionmentioning

confidence: 94%

“…Therefore, TxAS and TxA 2 receptor have been selected to be the indicators of TxA 2 synthesis and action in ample studies. Overexpression of TxAS has been documented to have a potential role in promoting the progression of many types of cancers (Nie et al, 2004;Sakai et al, 2006;Moussa et al, 2008a;Leung et al, 2009;Cathcart et al, 2010). In addition to TxAS, the important role of TxA 2 receptor in tumorigenesis and cancer progression has emerged (Sakai et al, 2006;Wei et al, 2007;Li and Tai, 2009;Cathcart et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

“…Overexpression of TxAS has been documented to have a potential role in promoting the progression of many types of cancers (Nie et al, 2004;Sakai et al, 2006;Moussa et al, 2008a;Leung et al, 2009;Cathcart et al, 2010). In addition to TxAS, the important role of TxA 2 receptor in tumorigenesis and cancer progression has emerged (Sakai et al, 2006;Wei et al, 2007;Li and Tai, 2009;Cathcart et al, 2010). Particularly, we have previously demonstrated that inhibition of TxAS results in the p27-related induction of cell death or apoptosis in both human non-small cell lung cancer (NSCLC) and small cell lung cancer (SCLC) cells (Leung et al, 2009), and other authors have recently reported that the activation of TxA 2 receptor induces cell proliferation in NSCLC cells (Li and Tai, 2009).…”

Section: Introductionmentioning

confidence: 99%

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4-Methylnitrosamino-1-3-pyridyl-1-butanone (NNK) promotes lung cancer cell survival by stimulating thromboxane A2 and its receptor

Huang

Hsin

et al. 2010

Oncogene

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The role of thromboxane A 2 (TxA 2 ) in smokingassociated lung cancer is poorly understood. This study was conducted to study the role of TxA 2 in smoking carcinogen 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone (NNK)-promoted cell survival and growth in human lung cancer cells. We found that NNK increased TxA 2 synthase (TxAS) expression and thromboxane B 2 (TxB 2 ) generation in cultured lung cancer cells, the result of which was supported by the increased level of TxAS in lung cancer tissues of smokers. Both TxAS-specific inhibitor furegrelate and TxA 2 receptor antagonist SQ29548 completely blocked NNK-mediated cell survival and growth via inducting apoptosis. TxA 2 receptor agonist U46619 reconstituted a near-full survival and growth response to NNK when TxAS was inhibited, affirming the role of TxA 2 receptor in NNK-mediated cell survival and growth. Suppression of cyclic adenosine monophosphate response element binding protein (CREB) activity by its small interference RNA blocked the effect of NNK. Phosphatidylinositol 3-kinase (PI3K)/Akt and extracellular signal-regulated kinase (ERK) also had a positive role. Altogether, our results have revealed that NNK stimulates TxA 2 synthesis and activates its receptor in lung cancer cells. The increased TxA 2 may then activate CREB through PI3K/Akt and extracellular ERK pathways, thereby contributing to the NNK-promoted survival and growth of lung cancer cells.

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Section: Discussionsupporting

confidence: 83%

Section: Discussionmentioning

confidence: 94%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

4-Methylnitrosamino-1-3-pyridyl-1-butanone (NNK) promotes lung cancer cell survival by stimulating thromboxane A2 and its receptor

Huang

Hsin

et al. 2010

Oncogene

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“…It has been known that PGD 2 and PGI 2 are anticarcinogenic agents (Keith et al, 2004;Park et al, 2007;Cathcart et al, 2010). PGD 2 is rapidly metabolized to 15-deoxy-D 12,14 -PGJ 2 , which inhibits tumor growth via a peroxisome proliferator-activated receptor g (PPARg)-dependent or -independent pathway (Scher and Pillinger, 2005;Mansure et al, 2009).…”

Section: Resultsmentioning

confidence: 99%

Microsomal prostaglandin E synthase-1 is involved in multiple steps of colon carcinogenesis

et al. 2011

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Accumulating evidence indicates that cyclooxygenase (COX)-2-derived prostaglandin (PG) E 2 is involved in the development of various tumors, including colorectal cancer. However, the precise contribution of microsomal PGE synthase (mPGES)-1, a terminal enzyme that acts downstream of COX-2 in the PGE 2 -biosynthetic pathway, to multiple processes of tumor development is not yet fully understood. Here, we show the pro-tumorigenic role of mPGES-1 in chemical carcinogen-induced colon carcinogenesis and intrasplenic tumor transplantation models. Genetic deletion of mPGES-1 significantly reduced both the total number and size of colorectal polyps at 18 weeks after azoxymethane administration with reduced nuclear translocation of b-catenin, altered expression profiles of chemokines/cytokines and increased production of antitumorigenic PGs, prostaglandin D 2 and prostacyclin in tumor tissues. At an early stage (6 weeks), mPGES-1 deficiency significantly reduced the number of aberrant crypt foci, while its transgenic overexpression increased the number. Furthermore, the growth of intrasplenically transplanted tumor cells was suppressed in mPGES-1 knockout (KO) mice. Co-culture of tumor cells with bone marrow-derived macrophages (BM-MUs) isolated from wild-type (WT) mice resulted in the induction of mPGES-1 in BM-MUs and increased the growth of tumor cells in vitro, whereas mPGES-1-null BM-MUs failed to facilitate tumor growth. The adoptive transfer of WT BM-MUs into mPGES-1 KO mice restored the growth of transplanted tumor cells, indicating that mPGES-1 in MUs is important for the growth of adjacent tumor cells. Taken together, our findings suggest that the inhibition of mPGES-1 is an alternative therapeutic target for colorectal and possibly other cancers.

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A new insight into subinteractomes of functional antagonists: Thromboxane (CYP5A1) and prostacyclin (CYP8A1) synthases

Ершов

Yablokov

Zgoda

et al. 2021

Cell Biology International

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The current article aims to summarize all possible spectrum of protein–protein interactions for thromboxane A synthase (CYP5A1) and prostacyclin synthase (CYP8A1). These enzymes metabolize the same substrate (prostaglandin H2) and can participate in cardiovascular, inflammatory, immune processes, and apoptosis modulation, as well as significantly influence the risk of cancers. Binary protein–protein and multiprotein complexes are of great importance in enzyme‐regulating and signal‐transduction pathways. However, protein partners of CYP5A1 and CYP8A1 are not yet fully identified, although both synthases are considered as prospective drug targets. At least 36 novel protein partners of CYP5A1 and CYP8A1 were revealed from different tissue types using an approach based on affinity isolation and mass spectrometry. Enrichment analysis showed that these proteins have different molecular functions: folding (refolding), unfolded protein and chaperon binding, protein transport (export/import), posttranslational modification, protein domain‐specific binding, antioxidant activity, and glutathione homeostasis. A significant part of them, belonging to molecular chaperones, were common partners for CYP5A1 and CYP8A1, while other proteins were unique with the tissue‐dependent distribution. New aspects of CYP5A1 and CYP8A1 interactomics and hetero‐complex formation with different protein partners, including cytochrome P450s are discussed.

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The role of prostacyclin synthase and thromboxane synthase signaling in the development and progression of cancer

Cited by 48 publications

References 173 publications

4-Methylnitrosamino-1-3-pyridyl-1-butanone (NNK) promotes lung cancer cell survival by stimulating thromboxane A2 and its receptor

4-Methylnitrosamino-1-3-pyridyl-1-butanone (NNK) promotes lung cancer cell survival by stimulating thromboxane A2 and its receptor

Microsomal prostaglandin E synthase-1 is involved in multiple steps of colon carcinogenesis

A new insight into subinteractomes of functional antagonists: Thromboxane (CYP5A1) and prostacyclin (CYP8A1) synthases

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