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分析白细胞介素-15 基因敲除小鼠的子宫基因表达,揭示了子宫自然杀伤细胞在蜕膜化和相关血管生成中不起主要作用。

Analysis of uterine gene expression in interleukin-15 knockout mice reveals uterine natural killer cells do not play a major role in decidualization and associated angiogenesis.

机构信息

Department of Physiology, Southern Illinois University School of Medicine, Carbondale, Illinois 62901, USA.

出版信息

Reproduction. 2012 Mar;143(3):359-75. doi: 10.1530/REP-11-0325. Epub 2011 Dec 20.

Abstract

During decidualization, uterine natural killer (uNK) cells are the most abundant immune cell types found in the uterus. Although it is well known that they play key roles in spiral arteriole modification and the maintenance of decidual integrity seen after mid-pregnancy, their roles in the differentiation of decidual cells and accompanying angiogenesis during the process of decidualization is less well characterized. To address this, we used whole-genome Illumina BeadChip analysis to compare the gene expression profiles in implantation segments of the uterus during decidualization on day 7.5 of pregnancy between wild-type and uNK cell-deficient (interleukin-15-knockout) mice. We found almost 300 differentially expressed genes and verified the differential expression of ~60 using quantitative RT-PCR. Notably, there was a lack of differential expression of genes involved in decidualization and angiogenesis and this was also verified by quantitative RT-PCR. Similar endothelial cell densities and proliferation indices were also found in the endometrium between the implantation site tissues of wild-type and knockout mice undergoing decidualization. Overall, the results of this study reveal that uNK cells likely do not play a major role in decidualization and accompanying angiogenesis during implantation. In addition, the study identifies a large number of genes whose expression in implantation-site uterine tissue during decidualization depends on interleukin-15 expression in mice.

摘要

在蜕膜化过程中,子宫自然杀伤(uNK)细胞是子宫中最丰富的免疫细胞类型。尽管众所周知它们在螺旋动脉改建和妊娠中期后维持蜕膜完整性方面发挥着关键作用,但它们在蜕膜细胞分化和伴随的血管生成中的作用在蜕膜化过程中还不太清楚。为了解决这个问题,我们使用全基因组 Illumina BeadChip 分析比较了妊娠第 7.5 天蜕膜化过程中子宫植入部位中野生型和 uNK 细胞缺陷(白细胞介素 15 敲除)小鼠之间的基因表达谱。我们发现了近 300 个差异表达基因,并使用定量 RT-PCR 验证了约 60 个基因的差异表达。值得注意的是,涉及蜕膜化和血管生成的基因表达没有差异,这也通过定量 RT-PCR 得到了验证。在经历蜕膜化的野生型和敲除小鼠的植入部位组织中,子宫内膜中的内皮细胞密度和增殖指数也相似。总体而言,这项研究的结果表明,uNK 细胞在植入期间的蜕膜化和伴随的血管生成中可能不起主要作用。此外,该研究还鉴定出大量在蜕膜化期间在植入部位子宫组织中表达的基因,其表达依赖于小鼠中白细胞介素 15 的表达。

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