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妊娠和分娩期间子宫肌层 AP-1 蛋白的差异表达。

Differential expression of myometrial AP-1 proteins during gestation and labour.

机构信息

Lunenfeld Tanenbaum Research Institute, Mount Sinai Hospital, Toronto, Ontario, Canada.

Department of Physiology, University of Toronto, Toronto, Ontario, Canada.

出版信息

J Cell Mol Med. 2018 Jan;22(1):452-471. doi: 10.1111/jcmm.13335. Epub 2017 Sep 25.

Abstract

Preterm labour (PTL) is a leading cause of perinatal mortality and postnatal morbidity. Contractions of the uterine muscle (myometrium) that determine the onset of labour depend on the expression of contraction-associated proteins (CAPs, i.e. connexin43) regulated by dimeric AP-1 transcription factors. Here, we examined subcellular (by immunoblotting) and tissue expression (by immunohistochemistry) of myometrial AP-1 proteins (cJUN, JUNB, JUND, cFOS, FOSB, FRA1, FRA2) throughout gestation and TL in different species (mouse, rat and human). To identify the critical AP-1 members associated with preterm birth, we studied their expression in mouse model of 'infectious' (LPS-induced) and 'sterile' (RU486-induced) PTL. We found that (1) myometrial AP-1 composition is preserved in vivo between different species (rodents and human) indicating that Fos/Jun heterodimer (i.e. FRA2/JUND) may be indispensable for labour initiation. (2) Our in vivo study using murine models of gestation shows that there is a similarity in the myometrial AP-1 protein composition during TL and pathological PTL of different aetiology suggesting the involvement of similar molecular machinery in the induction of labour. (3) This study is first comprehensive protein analysis of seven AP-1 members in human labouring versus non-labouring myometrium, showing their cellular expression and tissue distribution in relation to labour status.

摘要

早产(PTL)是围产期死亡和产后发病的主要原因。决定分娩开始的子宫肌肉(子宫肌)收缩取决于收缩相关蛋白(CAPs,即连接蛋白 43)的表达,这些蛋白受二聚体 AP-1 转录因子调节。在这里,我们检查了不同物种(小鼠、大鼠和人类)整个妊娠期和 TL 中子宫肌 AP-1 蛋白(cJUN、JUNB、JUND、cFOS、FOSB、FRA1、FRA2)的亚细胞(通过免疫印迹)和组织表达(通过免疫组织化学)。为了确定与早产相关的关键 AP-1 成员,我们研究了它们在“感染性”(LPS 诱导)和“无菌性”(RU486 诱导)PTL 小鼠模型中的表达。我们发现:(1)不同物种(啮齿动物和人类)之间子宫肌 AP-1 组成在体内保持不变,表明 Fos/Jun 异二聚体(即 FRA2/JUND)可能对分娩开始是不可或缺的。(2)我们使用妊娠小鼠模型进行的体内研究表明,在 TL 和不同病因的病理性 PTL 期间,子宫肌 AP-1 蛋白组成具有相似性,这表明在诱导分娩中涉及类似的分子机制。(3)这项研究是首次对人类分娩与非分娩子宫肌中的七个 AP-1 成员进行全面的蛋白质分析,显示了它们与分娩状态相关的细胞表达和组织分布。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/09ae/5742715/f7cb18b2bb48/JCMM-22-452-g001.jpg

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