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造血前列腺素 D 合酶:一种依赖 ESR1 的输卵管上皮细胞合成酶。

Hematopoetic prostaglandin D synthase: an ESR1-dependent oviductal epithelial cell synthase.

机构信息

Department of Animal and Food Sciences, University of Kentucky, Lexington, Kentucky 40546, USA.

出版信息

Endocrinology. 2012 Apr;153(4):1925-35. doi: 10.1210/en.2011-1900. Epub 2012 Feb 28.

Abstract

Oviductal disease is a primary cause of infertility, a problem that largely stems from excessive inflammation of this key reproductive organ. Our poor understanding of the mechanisms regulating oviductal inflammation restricts our ability to diagnose, treat, and/or prevent oviductal disease. Using mice, our objective was to determine the spatial localization, regulatory mechanism, and functional attributes of a hypothesized regulator of oviductal inflammation, the hematopoietic form of prostaglandin D synthase (HPGDS). Immunohistochemistry revealed specific localization of HPGDS to the oviduct's epithelium. In the isthmus, expression of HPGDS was consistent. In the ampulla, expression of HPGDS appeared dependent upon stage of the estrous cycle. HPGDS was expressed in the epithelium of immature and cycling mice but not in the oviducts of estrogen receptor α knockouts. Two receptor subtypes bind PGD₂: PGD₂ receptor and G protein-coupled receptor 44. Expression of mRNA for Ptgdr was higher in the epithelial cells (EPI) than in the stroma (P < 0.05), whereas mRNA for Gpr44 was higher in the stroma than epithelium (P < 0.05). Treatment of human oviductal EPI with HQL-79, an inhibitor of HPGDS, decreased cell viability (P < 0.05). Treatment of mice with HQL-79 increased mRNA for chemokine (C-C motif) ligands 3, 4, and 19; chemokine (C-X-C motif) ligands 11 and 12; IL-13 and IL-17B; and TNF receptor superfamily, member 1b (P < 0.02 for each mRNA). Overall, these results suggest that HPGDS may play a role in the regulation of inflammation and EPI health within the oviduct.

摘要

输卵管疾病是不孕的主要原因,这主要是由于这个关键生殖器官的过度炎症引起的。我们对调节输卵管炎症的机制了解甚少,这限制了我们诊断、治疗和/或预防输卵管疾病的能力。我们使用小鼠来确定假设的输卵管炎症调节剂——造血型前列腺素 D 合酶(HPGDS)的空间定位、调节机制和功能属性。免疫组织化学显示 HPGDS 特异性定位于输卵管上皮。在峡部,HPGDS 的表达是一致的。在壶腹部,HPGDS 的表达似乎依赖于发情周期的阶段。HPGDS 在未成熟和发情期小鼠的上皮细胞中表达,但在雌激素受体 α 敲除小鼠的输卵管中不表达。两种受体亚型结合 PGD₂:PGD₂受体和 G 蛋白偶联受体 44。Ptgdr 的 mRNA 在上皮细胞(EPI)中的表达高于基质(P < 0.05),而 Gpr44 的 mRNA 在基质中的表达高于上皮细胞(P < 0.05)。用 HPGDS 抑制剂 HQL-79 处理人输卵管上皮细胞会降低细胞活力(P < 0.05)。用 HQL-79 处理小鼠会增加趋化因子(C-C 基序)配体 3、4 和 19;趋化因子(C-X-C 基序)配体 11 和 12;IL-13 和 IL-17B;和 TNF 受体超家族成员 1b(每种 mRNA 的 P < 0.02)。总的来说,这些结果表明 HPGDS 可能在调节输卵管内炎症和上皮细胞健康方面发挥作用。

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