Microarray expression profiling reveals candidate genes for human uterine receptivity.

Linda C Giudice
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引用次数: 87

Abstract

The endometrium undergoes cyclic changes in response to circulating ovarian steroid hormones as it prepares for implantation. This dynamic tissue is well suited to microarray expression profiling for elucidation of molecular players participating in the maturation of the endometrium and during the process of implantation. Recent advances in sequencing the human and mouse genomes and the availability of microarray technology and bioinformatic analyses have made elucidating these molecular participants and dialogs a reality. Analysis of the window of implantation, a temporal and spatially unique period in which the endometrium is receptive to embryonic implantation, has revealed numerous processes to be occurring simultaneously or sequentially. These include cell cycle regulation, angiogenesis, immune modulation of implantation, defense mechanisms put into place by antibacterial agents and detoxicants, secretion of unique products, transport of ions and water, growth factor actions, steroid hormone action and metabolism, and production of extracellular matrix proteins, unique cell surface glycoproteins, and a variety of transcription factors, to name a few. Several groups have recently conducted studies with human endometrium, and remarkable similarities exist with mouse. Also, many genes and gene families involved in the unique differentiation process of stromal cell decidualization are conserved. In addition, infertility associated with endometriosis is partly implantation-based, and gene profiling of such tissue during the window of implantation has revealed additional insight into mechanisms underlying infertility in this disorder. Global profiling of genes in the endometrium, decidua, and at the interface between the trophoblast and the decidua, has provided remarkable in sight into endometrial maturation and implantation.

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微阵列表达谱揭示了人类子宫接受性的候选基因。
子宫内膜在为着床做准备时,对循环的卵巢类固醇激素作出反应而发生周期性变化。这种动态组织非常适合用于微阵列表达谱分析,以阐明参与子宫内膜成熟和着床过程中的分子参与者。人类和小鼠基因组测序的最新进展以及微阵列技术和生物信息学分析的可用性使得阐明这些分子参与者和对话成为现实。着床窗口是一个时间和空间上独特的时期,在这个时期子宫内膜可以接受胚胎着床,对着床窗口的分析揭示了许多过程同时或依次发生。这些包括细胞周期调节、血管生成、植入的免疫调节、抗菌剂和解毒剂的防御机制、独特产物的分泌、离子和水的运输、生长因子的作用、类固醇激素的作用和代谢、细胞外基质蛋白的产生、独特的细胞表面糖蛋白和各种转录因子,等等。几个研究小组最近对人类子宫内膜进行了研究,发现与小鼠子宫内膜有显著的相似之处。此外,许多参与基质细胞脱个体化独特分化过程的基因和基因家族是保守的。此外,与子宫内膜异位症相关的不孕症部分是基于植入的,在植入窗口期间对这些组织的基因谱分析揭示了这种疾病中不孕症的潜在机制。子宫内膜、蜕膜以及滋养细胞和蜕膜交界面基因的全局分析,为子宫内膜成熟和着床提供了显著的视角。
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