Prostaglandins and the regulation of tumor growth.

Journal of environmental pathology, toxicology and oncology : official organ of the International Society for Environmental Toxicology and Cancer Pub Date : 2002-01-01 DOI:10.1615/JENVIRONPATHOLTOXICOLONCOL.V21.I2.20

D. Bishop-Bailey, S. Calatayud, T. Warner, T. Hla, J. Mitchell

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引用次数: 79

Abstract

Increased expression of inducible cyclooxygenase (COX-2) is associated with a wide variety of tumors. In addition, inhibitors of COX have shown a great deal of promise in vitro and in animal models as potential antitumor therapies. COX enzymes use the substrate arachidonic acid to produce prostaglandin (PG)H2, the precursor to all the prostanoids. Therefore, the release of individual prostanoids depends on the abundance and functional coupling to individual PG synthase isoenzymes. Colony stimulating factors (CSFs) are also potential antitumor agents via their ability to augment the immune response. When COX-2 is expressed, the CSF, granulocyte macrophage (GM)-CSF, and granulocyte (G)-CSF are exquisitely sensitive to endogenous PGs. In addition, the ability of COX-2 to suppress GM-CSF release is mediated via traditional IP/EP prostanoid receptors linked to cAMP-dependent pathways. Therefore, inhibition of COX-2 in tumors may have the important side effect of enhancing the immune response. Recently, novel signaling pathways for PG derivatives have been discovered; in particular the PGD2 dehydration product 15-deoxy-delta(12,14)-(15d)-PGJ2 was identified as a ligand for the nuclear receptor/transcription factor, peroxisome proliferator-activated receptor (PPAR)-gamma. PPARgamma is present at high levels in a number of tumors, and is also present in endothelial cells. 15d-PGJ2 as well as other nonprostanoid PPARgamma ligands are antitumor, and antiangiogenic, by dramatically inhibiting the growth of tumor cells and endothelial cells by either causing terminal differentiation, and/or by inducing apoptosis. We have recently found that, in addition to IP and EP ligands generated by COX-2, PPARgamma ligands similarly inhibit GM-CSF release. Effecting individual prostanoid pathways at the level of COX expression, profile of PG products produced or selective PG receptor activation may produce novel therapies, either dependent or independent of CSF release, to target cancers.

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前列腺素与肿瘤生长的调控。

诱导型环氧合酶(COX-2)的表达增加与多种肿瘤有关。此外，COX抑制剂在体外和动物模型中作为潜在的抗肿瘤疗法显示出很大的希望。COX酶利用底物花生四烯酸产生前列腺素(PG)H2，这是所有前列腺素的前体。因此，单个前列腺素的释放取决于与单个PG合成酶同工酶的丰度和功能偶联。集落刺激因子(csf)通过其增强免疫反应的能力也是潜在的抗肿瘤药物。当COX-2表达时，CSF、粒细胞巨噬细胞(GM)-CSF和粒细胞(G)-CSF对内源性pg非常敏感。此外，COX-2抑制GM-CSF释放的能力是通过与camp依赖途径相关的传统IP/EP前列腺素受体介导的。因此，抑制肿瘤中的COX-2可能具有增强免疫应答的重要副作用。近年来，PG衍生物的新信号通路被发现;特别是PGD2脱水产物15-脱氧- δ (12,14)-(15d)- pgj2被鉴定为核受体/转录因子，过氧化物酶体增殖体激活受体(PPAR)- γ的配体。PPARgamma在许多肿瘤中含量很高，内皮细胞中也有。15d-PGJ2和其他非前列腺素类PPARgamma配体具有抗肿瘤和抗血管生成的作用，它们通过引起终末分化和/或诱导细胞凋亡来显著抑制肿瘤细胞和内皮细胞的生长。我们最近发现，除了COX-2产生的IP和EP配体外，PPARgamma配体也同样抑制GM-CSF的释放。在COX表达水平上影响单个前列腺素通路，产生PG产物的谱或选择性PG受体激活可能产生依赖或独立于CSF释放的新疗法，以靶向癌症。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Journal of environmental pathology, toxicology and oncology : official organ of the International Society for Environmental Toxicology and Cancer

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