首页> 美国卫生研究院文献>Clinical Molecular Pathology >Temporal and spatial expression of connective tissue growth factor (CCN2; CTGF) and transforming growth factor β type 1 (TGF-β1) at the utero–placental interface during early pregnancy in the pig
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Temporal and spatial expression of connective tissue growth factor (CCN2; CTGF) and transforming growth factor β type 1 (TGF-β1) at the utero–placental interface during early pregnancy in the pig

机译:猪早期妊娠期间子宫-胎盘界面结缔组织生长因子(CCN2; CTGF)和转化生长因子β1型(TGF-β1)的时空表达

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摘要

>Aims: To determine the localisation and distribution of connective tissue growth factor (CCN2; CTGF) and transforming growth factor β type 1 (TGF-β1) in uterine tissues from cycling and early pregnant pigs.>Methods: In situ hybridisation and immunohistochemistry were used to localise CCN2 (CTGF) or TGF-β1 in uteri obtained from gilts on days 0, 5, 10, 12, 15, and 18 of the oestrous cycle or days 10, 12, 14, 16, 17, and 21 of gestation.>Results: In cycling animals, CCN2 (CTGF) mRNA and protein were abundant in luminal epithelial cells (LECs) and glandular epithelial cells (GECs), with lesser amounts in stromal fibroblasts and little or none in endothelial cells. A similar pattern of staining was seen up to day 10 of pregnancy, except that overall staining intensities for CCN2 (CTGF) mRNA or protein were higher and that stromal and endothelial cells were CCN2 (CTGF) positive. However, on days 12–17 there was a striking decrease in the amount of CCN2 (CTGF) in LECs at the utero–conceptus interface, which was associated with maternal stromal matrix reorganisation and the onset of subepithelial neovascularisation. This differential distribution of CCN2 (CTGF) was localised to those LECs that were in close proximity to or in apposition with trophoblast cells. This decrease in CCN2 (CTGF) staining was transient in nature and high amounts of CCN2 (CTGF) were again apparent in LECs on days 17–21, when endometrial neovascularisation and matrix remodelling were complete. The expression of uterine TGF-β1 was comparable to that of CCN2 (CTGF) at most stages of the oestrous cycle or early pregnancy. Pre-elongation blastocysts recovered on day 10 were positive for both CCN2 (CTGF) and TGF-β1 in the extra-embryonic trophectoderm, endoderm, and inner cell mass. On day 12, trophectoderm expressed low amounts of TGF-β1 mRNA and non-detectable amounts of TGF-β1 protein or CCN2 (CTGF) mRNA or protein. By days 17–21, the expression of both growth factors in the extra-embyronic/placental membranes increased and frequently exceeded that seen in LECs.>Conclusions: The pattern of CCN2 (CTGF) production during the initial attachment phase supports a role for this factor in stromal remodelling and neovascularisation, although alternative functions at later stages such as epithelial–epithelial interactions are also possible. In most major cell types in the uterus or utero–placental unit, CCN2 (CTGF) expression was highly correlated with that of TGF-β1, indicating that CCN2 (CTGF) may mediate some of the functions of TGF-β in the reproductive tract during the oestrous cycle and pregnancy. The data further highlight epithelium as an important source of CCN2 (CTGF) in the regulation of uterine function.
机译:>目的:确定循环和早孕猪子宫组织中结缔组织生长因子(CCN2; CTGF)和转化生长因子β1型(TGF-β1)的定位和分布。>方法:采用原位杂交和免疫组化技术,在雌性周期的第0、5、10、12、15和18天或第10天,从小母猪获得的子宫中定位CCN2(CTGF)或TGF-β1。 >结果:在骑自行车的动物中,腔上皮细胞(LEC)和腺上皮细胞(GEC)中的CCN2(CTGF)mRNA和蛋白质丰富,基质成纤维细胞的数量较少,内皮细胞的数量很少或没有。直到怀孕的第10天都观察到类似的染色模式,除了CCN2(CTGF)mRNA或蛋白质的总体染色强度更高,以及基质和内皮细胞CCN2(CTGF)阳性。然而,在第12-17天,子宫-概念界面的LEC中CCN2(CTGF)的数量显着减少,这与母体基质基质重组和上皮下新生血管形成有关。 CCN2(CTGF)的这种差异分布被定位在与滋养层细胞紧邻或并列的那些LEC。 CCN2(CTGF)染色的这种降低本质上是短暂的,当子宫内膜新生血管形成和基质重塑完成时,在第17-21天,在LEC中再次出现大量的CCN2(CTGF)。子宫TGF-β1的表达在发情周期或早期妊娠的大多数阶段与CCN2(CTGF)相当。在第10天恢复的伸长前胚泡在胚外滋养外胚层,内胚层和内细胞团中CCN2(CTGF)和TGF-β1均为阳性。在第12天,滋养外胚层表达低水平的TGF-β1mRNA和不可检测的TGF-β1蛋白或CCN2(CTGF)mRNA或蛋白。到第17-21天时,两种生长因子在胎膜外/胎盘膜中的表达增加,并经常超过LEC中的表达。>结论:在初始附着过程中CCN2(CTGF)产生的模式阶段支持这一因素在基质重塑和新血管形成中的作用,尽管在以后阶段的替代功能如上皮-上皮相互作用也是可能的。在子宫或子宫-胎盘单位的大多数主要细胞类型中,CCN2(CTGF)的表达与TGF-β1高度相关,这表明CCN2(CTGF)可能介导TGF-β在生殖道中的某些功能。发情周期和怀孕。数据进一步强调了上皮是调节子宫功能中CCN2(CTGF)的重要来源。

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