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Selective Inhibition of Prostaglandin E2 Receptors EP2 and EP4 Induces Apoptosis of Human Endometriotic Cells through Suppression of ERK1/2 AKT NFκB and β-Catenin Pathways and Activation of Intrinsic Apoptotic Mechanisms

机译：前列腺素E2受体EP2和EP4的选择性抑制通过抑制ERK1 / 2AKTNFκB和β-Catenin途径以及激活内在凋亡机制诱导人子宫内膜异位细胞凋亡。

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Endometriosis is a benign chronic gynecological disease of reproductive-age women characterized by the presence of functional endometrial tissues outside the uterine cavity. It is an estrogen-dependent disease. Current treatment modalities to inhibit biosynthesis and actions of estrogen compromise menstruation, pregnancy, and the reproductive health of women and fail to prevent reoccurrence of disease. There is a critical need to identify new specific signaling modules for non-estrogen-targeted therapies for endometriosis. In our previous study, we reported that selective inhibition of cyclooxygenase-2 prevented survival, migration, and invasion of human endometriotic epithelial and stromal cells, which was due to decreased prostaglandin E2 (PGE2) production. In this study, we determined mechanisms through which PGE2 promoted survival of human endometriotic cells. Results of the present study indicate that 1) PGE2 promotes survival of human endometriotic cells through EP2 and EP4 receptors by activating ERK1/2, AKT, nuclear factor-κB, and β-catenin signaling pathways; 2) selective inhibition of EP2 and EP4 suppresses these cell survival pathways and augments interactions between proapoptotic proteins (Bax and Bad) and antiapoptotic proteins (Bcl-2/Bcl-XL), facilitates the release of cytochrome c, and thus activates caspase-3/poly (ADP-ribose) polymerase-mediated intrinsic apoptotic pathways; and 3) these PGE2 signaling components are more abundantly expressed in ectopic endometriosis tissues compared with eutopic endometrial tissues during the menstrual cycle in women. These novel findings may provide an important molecular framework for further evaluation of selective inhibition of EP2 and EP4 as potential therapy, including nonestrogen target, to expand the spectrum of currently available treatment options for endometriosis in women.

机译：子宫内膜异位症是一种生殖年龄妇女的良性慢性妇科疾病，其特征是子宫腔外存在功能性子宫内膜组织。它是雌激素依赖性疾病。当前抑制雌激素的生物合成和作用的治疗方式损害了妇女的月经，怀孕和生殖健康，无法预防疾病的复发。迫切需要为子宫内膜异位症的非雌激素靶向疗法确定新的特异性信号传导模块。在我们之前的研究中，我们报道了选择性抑制环氧合酶2阻止了人类子宫内膜异位上皮细胞和基质细胞的存活，迁移和侵袭，这是由于前列腺素E2（PGE2）生成减少所致。在这项研究中，我们确定了PGE2促进人类子宫内膜异位细胞存活的机制。本研究结果表明：1）PGE2通过激活ERK1 / 2，AKT，核因子-κB和β-catenin信号通路，通过EP2和EP4受体促进人子宫内膜异位细胞的存活； 2）选择性抑制EP2和EP4可抑制这些细胞存活途径并增强促凋亡蛋白（Bax和Bad）与抗凋亡蛋白（Bcl-2 / Bcl-XL）之间的相互作用，促进细胞色素c的释放，从而激活caspase-3 / poly（ADP-核糖）聚合酶介导的内在凋亡途径；（3）与女性经期子宫内膜组织相比，这些PGE2信号传导成分在异位子宫内膜异位组织中的表达更为丰富。这些新发现可能为进一步评估对EP2和EP4的选择性抑制作为潜在的治疗方法（包括非雌激素靶标）提供了重要的分子框架，从而扩大了妇女子宫内膜异位症当前可用治疗方案的范围。

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期刊名称 Molecular Endocrinology
作者
Sakhila K. Banu; 1; JeHoon Lee; 1; V. O. Speights Jr.; Anna Starzinski-Powitz; Joe A. Arosh;
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作者单位

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年(卷),期 -1(23),8
年度 -1
页码 1291–1305
总页数 6
原文格式 PDF
正文语种
中图分类分子生物学;
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专利

1. Selective inhibition of prostaglandin E2 receptors EP2 and EP4 inhibits adhesion of human endometriotic epithelial and stromal cells through suppression of integrin-mediated mechanisms [J] . LeeJ., BanuS.K., BurghardtR.C., Biology of Reproduction: Offical Journal of the Society for the Study of Reproduction . 2013,第3期

机译：选择性抑制前列腺素E2受体EP2和EP4通过抑制整联蛋白介导的机制来抑制人内膜静脉肌上皮和基质细胞的粘附
2. Selective inhibition of prostaglandin E2 receptors EP2 and EP4 inhibits adhesion of human endometriotic epithelial and stromal cells through suppression of integrin-mediated mechanisms [J] . LeeJ., BanuS.K., BurghardtR.C., Biology of Reproduction: Offical Journal of the Society for the Study of Reproduction . 2013,第3期

机译：选择性抑制前列腺素E2受体EP2和EP4通过抑制整联蛋白介导的机制来抑制人内膜静脉肌上皮和基质细胞的粘附
3. Selective inhibition of prostaglandin E2 receptors EP2 and EP4 inhibits invasion of human immortalized endometriotic epithelial and stromal cells through suppression of metalloproteinases. [J] . Lee J, Banu SK, Subbarao T, Molecular and Cellular Endocrinology . 2011,第1a2期

机译：前列腺素E2受体EP2和EP4的选择性抑制通过抑制金属蛋白酶抑制人类永生化的子宫内膜异位上皮和基质细胞的侵袭。
4. Caspase Activation and Extracellular Signal-Regulated Kinase/Akt Inhibition Were Involved in Luteolin-Induced Apoptosis in Lewis Lung Carcinoma Cells [C] . JIN-HYUNG KIM, EUN-OK LEE, HYO-JUNG LEE, Meeting on Cell Signaling World: Signal Transduction Pathways as Therapeutic Targets . 2007

机译：半胱氨酸天冬氨酸蛋白酶激活和细胞外信号调节激酶/ Akt抑制涉及路易斯-肺癌细胞中木犀草素诱导的细胞凋亡。
5. Roles of cellular FLICE-inhibitory protein (c-FLIP) and PI3K/Akt in Fas (CD95)-induced NF-kappaB activation and apoptosis through death effector domains. [D] . Lu, Bin. 2005

机译：细胞FLICE抑制蛋白（c-FLIP）和PI3K / Akt在Fas（CD95）诱导的NF-κB活化和细胞凋亡中通过死亡效应域的作用。
6. Selective Inhibition of Prostaglandin E2 Receptors EP2 and EP4 Inhibits Adhesion of Human Endometriotic Epithelial and Stromal Cells Through Suppression of Integrin-Mediated Mechanisms [O] . JeHoon Lee, Sakhila K. Banu, Robert C. Burghardt, -1

机译：选择性抑制前列腺素E 2受体EP 2和EP 4通过抑制整合素介导的机制抑制人子宫内膜异位上皮和基质细胞的粘附。
7. Selective Inhibition of Prostaglandin E2 Receptors EP2 and EP4 Induces Apoptosis of Human Endometriotic Cells through Suppression of ERK1/2, AKT, NFκB, and β-Catenin Pathways and Activation of Intrinsic Apoptotic Mechanisms [O] . Sakhila K. Banu, JeHoon Lee, V. O. Speights, 2009

机译：选择性抑制前列腺素E2受体EP2和EP4通过抑制ERK1 / 2，AKT，NFκB和β-连环蛋白途径和固有凋亡机制的激活诱导人内膜静脉肌细胞的凋亡

Selective Inhibition of Prostaglandin E2 Receptors EP2 and EP4 Induces Apoptosis of Human Endometriotic Cells through Suppression of ERK1/2 AKT NFκB and β-Catenin Pathways and Activation of Intrinsic Apoptotic Mechanisms

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