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人黄体化颗粒细胞——人黄体的细胞模型

Human Luteinized Granulosa Cells-A Cellular Model for the Human Corpus Luteum.

作者信息

Bagnjuk Konstantin, Mayerhofer Artur

机构信息

Biomedical Center Munich (BMC), Cell Biology, Anatomy III, Ludwig-Maximilians-University (LMU), Planegg, Germany.

出版信息

Front Endocrinol (Lausanne). 2019 Jul 9;10:452. doi: 10.3389/fendo.2019.00452. eCollection 2019.

Abstract

In the ovary, the corpus luteum (CL) forms a temporal structure. Luteinized mural granulosa cells (GCs), which stem from the ruptured follicle, are the main cells of the CL. They can be isolated from follicular fluid of woman undergoing fertilization. In culture, human GCs are viable for several days and produce progesterone, yet eventually steroid production stops and GCs with increasing time in culture undergo changes reminiscent of the ones observed during the demise of the CL . This short review summarizes the general use of human GCs as a model for the primate CL and some of the data from our lab, which indicate that viability, functionality, survival and death of GCs can be regulated by local signal molecules (e.g., oxytocin and PEDF) and the extracellular matrix (e.g., via the proteoglycan decorin). We further summarize studies, which identified autophagocytotic events in human GCs linked to the activation of an ion channel. More recent studies identified a form of regulated cell death, namely necroptosis. This form of cell death may, in addition to apoptosis, contribute to the demise of the human CL. We believe that human GCs are a unique window into the human CL. Studies employing these cells may lead to the identification of molecular events and novel targets, which may allow to interfere with CL functions.

摘要

在卵巢中,黄体(CL)形成一种临时性结构。源自破裂卵泡的黄素化壁颗粒细胞(GCs)是黄体的主要细胞。它们可以从接受受精的女性的卵泡液中分离出来。在培养中,人颗粒细胞可存活数天并产生孕酮,但最终类固醇生成会停止,且随着培养时间的增加,颗粒细胞会发生一些变化,这些变化让人联想到在黄体退化过程中所观察到的变化。这篇简短的综述总结了人颗粒细胞作为灵长类黄体模型的一般用途以及我们实验室的一些数据,这些数据表明颗粒细胞的活力、功能、存活和死亡可受到局部信号分子(如催产素和PEDF)和细胞外基质(如通过蛋白聚糖核心蛋白聚糖)的调节。我们还总结了一些研究,这些研究确定了人颗粒细胞中与离子通道激活相关的自噬事件。最近的研究发现了一种程序性细胞死亡形式,即坏死性凋亡。除了凋亡之外,这种细胞死亡形式可能也导致了人黄体的退化。我们认为人颗粒细胞是了解人黄体的一个独特窗口。利用这些细胞进行的研究可能会导致识别分子事件和新的靶点,从而有可能干扰黄体功能。

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