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雌激素-巨噬细胞在女性生殖道稳态中的相互作用。

The estrogen-macrophage interplay in the homeostasis of the female reproductive tract.

机构信息

Department of Pharmacological and Biomolecular Sciences, Center of Excellence on Neurodegenerative Diseases, University of Milan, via Balzaretti, 9 Milan, Italy.

Humanitas Clinical and Research Center, Segrate, Italy.

出版信息

Hum Reprod Update. 2018 Nov 1;24(6):652-672. doi: 10.1093/humupd/dmy026.

Abstract

BACKGROUND

Estrogens are known to orchestrate reproductive events and to regulate the immune system during infections and following tissue damage. Recent findings suggest that, in the absence of any danger signal, estrogens trigger the physiological expansion and functional specialization of macrophages, which are immune cells that populate the female reproductive tract (FRT) and are increasingly being recognized to participate in tissue homeostasis beyond their immune activity against infections. Although estrogens are the only female gonadal hormones that directly target macrophages, a comprehensive view of this endocrine-immune communication and its involvement in the FRT is still missing.

OBJECTIVE AND RATIONALE

Recent accomplishments encourage a revision of the literature on the ability of macrophages to respond to estrogens and induce tissue-specific functions required for reproductive events, with the aim to envision macrophages as key players in FRT homeostasis and mediators of the regenerative and trophic actions of estrogens.

SEARCH METHODS

We conducted a systematic search using PubMed and Ovid for human, animal (rodents) and cellular studies published until 2018 on estrogen action in macrophages and the activity of these cells in the FRT.

OUTCOMES

Our search identified the remarkable ability of macrophages to activate biochemical processes in response to estrogens in cell culture experiments. The distribution at specific locations, interaction with selected cells and acquisition of distinct phenotypes of macrophages in the FRT, as well as the cyclic renewal of these properties at each ovarian cycle, demonstrate the involvement of these cells in the homeostasis of reproductive events. Moreover, current evidence suggests an association between estrogen-macrophage signaling and the generation of a tolerant and regenerative environment in the FRT, although a causative link is still missing.

WIDER IMPLICATIONS

Dysregulation of the functions and estrogen responsiveness of FRT macrophages may be involved in infertility and estrogen- and macrophage-dependent gynecological diseases, such as ovarian cancer and endometriosis. Thus, more research is needed on the physiology and pharmacological control of this endocrine-immune interplay.

摘要

背景

雌激素已知能协调生殖事件,并在感染和组织损伤后调节免疫系统。最近的研究结果表明,在没有任何危险信号的情况下,雌激素会触发巨噬细胞的生理扩张和功能特化,巨噬细胞是存在于女性生殖道(FRT)中的免疫细胞,它们越来越被认为除了对感染的免疫活性外,还参与组织稳态。尽管雌激素是唯一直接靶向巨噬细胞的女性性腺激素,但这种内分泌-免疫通讯及其在 FRT 中的参与仍缺乏全面的认识。

目的和理由

最近的成就鼓励对巨噬细胞对雌激素的反应能力以及诱导生殖事件所需的组织特异性功能的文献进行修订,目的是将巨噬细胞视为 FRT 稳态的关键参与者和雌激素的再生和营养作用的介导者。

搜索方法

我们使用 PubMed 和 Ovid 进行了系统搜索,以查找截至 2018 年发表的关于雌激素在巨噬细胞中的作用以及这些细胞在 FRT 中的活性的人类、动物(啮齿动物)和细胞研究文献。

结果

我们的搜索结果表明,巨噬细胞在细胞培养实验中具有激活雌激素相关生化过程的显著能力。FRT 中巨噬细胞的特定位置分布、与选定细胞的相互作用以及获得独特的表型,以及每个卵巢周期中这些特性的周期性更新,都证明了这些细胞参与了生殖事件的稳态。此外,目前的证据表明,雌激素-巨噬细胞信号与 FRT 中耐受和再生环境的产生之间存在关联,尽管仍缺乏因果关系。

更广泛的影响

FRT 巨噬细胞的功能和雌激素反应性失调可能与不孕以及雌激素和巨噬细胞依赖性妇科疾病有关,如卵巢癌和子宫内膜异位症。因此,需要对这种内分泌-免疫相互作用的生理学和药理学控制进行更多的研究。

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