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一项旨在鉴定早产和足月产人子宫肌层中差异基因表达的功能基因组学研究。

A functional genomic study to identify differential gene expression in the preterm and term human myometrium.

作者信息

Charpigny G, Leroy M-J, Breuiller-Fouché M, Tanfin Z, Mhaouty-Kodja S, Robin Ph, Leiber D, Cohen-Tannoudji J, Cabrol D, Barberis C, Germain G

机构信息

Physiologie Animale, INRA, Centre de Recherches de Jouy, 78352 Jouy en Josas cedex, France.

出版信息

Biol Reprod. 2003 Jun;68(6):2289-96. doi: 10.1095/biolreprod.102.013763. Epub 2003 Feb 5.

Abstract

The mechanisms that lead to the onset of human parturition are still unknown, although selected critical factors have been identified. To investigate the changes in myometrial gene expression associated with parturition, we used two macroarrays each containing 1176 different complementary human cDNA clones. Methods involving hierarchical clustering and conventional statistical analysis allowed us to generate a profile of genes expression at three stages of late pregnancy: preterm (29 wk amenorrhea); full term, not in labor (38 wk amenorrhea); and full term in labor (39 wk amenorrhea). Only 4% of the genes investigated were differentially expressed between the preterm and term groups (P < 0.05). These genes could be clustered as groups of either down-regulated or up-regulated transcripts. The changes in transcript abundance were particularly marked between the preterm and term stages of gestation, whereas the differences between term not in labor and term in labor were less pronounced. The parturition was characterized by a massive down-regulation of a large panel of developmental, cell adhesion molecule and proliferation-related genes, along with the up-regulation of inflammatory, contraction and apoptosis associated genes. We propose that the mechanisms of parturition consist primarily in the arrest of the processes of myometrial development, a step that might be essential to allow the uterus to recover appropriate contractile function before delivery.

摘要

导致人类分娩开始的机制仍然未知,尽管已经确定了一些关键因素。为了研究与分娩相关的子宫肌层基因表达变化,我们使用了两个宏阵列,每个宏阵列包含1176个不同的人类互补cDNA克隆。涉及层次聚类和传统统计分析的方法使我们能够生成妊娠晚期三个阶段的基因表达谱:早产(闭经29周);足月,未临产(闭经38周);以及足月临产(闭经39周)。在早产组和足月组之间,只有4%的研究基因存在差异表达(P<0.05)。这些基因可以聚类为下调或上调转录本组。转录本丰度的变化在妊娠的早产和足月阶段尤为明显,而未临产足月和临产足月之间的差异则不太明显。分娩的特征是大量发育、细胞粘附分子和增殖相关基因的下调,以及炎症、收缩和凋亡相关基因的上调。我们认为,分娩机制主要在于子宫肌层发育过程的停止,这一步骤对于使子宫在分娩前恢复适当的收缩功能可能至关重要。

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