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首页> 外文期刊>Cell and Tissue Research >The adhering junctions of valvular interstitial cells: molecular composition in fetal and adult hearts and the comings and goings of plakophilin-2 in situ, in cell culture and upon re-association with scaffolds
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The adhering junctions of valvular interstitial cells: molecular composition in fetal and adult hearts and the comings and goings of plakophilin-2 in situ, in cell culture and upon re-association with scaffolds

机译:瓣膜间质细胞的粘附连接:胎儿和成年心脏中的分子组成,以及原位,细胞培养中以及与支架重新结合后的plakophilin-2的来来去去

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摘要

The interstitial cells of cardiac valves represent one of the most frequent cell types in the mammalian heart. In order to provide a cell and molecular biological basis for the growth of isolated valvular interstitial cells (VICs) in cell culture and for the use in re-implantation surgery we have examined VICs in situ and in culture, in fetal, postnatal and adult hearts, in re-associations with scaffolds of extracellular matrix (ECM) material and decellularized heart valves. In all four mammalian species examined (human, bovine, porcine and ovine), the typical mesenchymal-type cell-cell adherens junctions (AJs) connecting VICs appear as normal N-cadherin based puncta adhaerentia. Their molecular ensemble, however, changes under various growth conditions insofar as plakophilin-2 (Pkp2), known as a major cytoplasmic plaque component of epithelial desmosomes, is recruited to and integrated in the plaques of VIC-AJs as a major component under growth conditions characterized by enhanced proliferation, i.e., in fetal heart valves and in cell cultures. Upon re-seeding onto decellularized heart valves or in stages of growth in association with artificial scaffolds, Pkp2 is — for the most part — lost from the AJs. As Pkp2 has recently also been detected in AJs of cardiac myxomata and diverse other mesenchymal tumors, the demonstrated return to the normal Pkp2-negative state upon re-association with ECM scaffolds and decellularized heart valves may now provide a safe basis for the use of cultured VICs in valve replacement surgery. Even more surprising, this type of transient acquisition of Pkp2 has also been observed in distinct groups of endothelial cells of the endocardium, where it seems to correspond to the cell type ready for endothelial–mesenchymal transition (EMT).
机译:心脏瓣膜的间质细胞代表哺乳动物心脏中最常见的细胞类型之一。为了为分离的瓣膜间质细胞(VIC)在细胞培养中的生长以及在再植入手术中的使用提供细胞和分子生物学基础,我们已经在胎儿,出生后和成年心脏中就地和在文化中检查了VIC ,与细胞外基质(ECM)材料支架和脱细胞的心脏瓣膜重新结合。在所检查的所有四个哺乳动物物种(人类,牛,猪和绵羊)中,连接VIC的典型间质型细胞-细胞粘附连接(AJ)均显示为正常的基于N-钙粘着蛋白的点状突水。然而,它们的分子集合在各种生长条件下会发生变化,因为被称为上皮桥粒主要细胞质斑块成分的plakophilin-2(Pkp2)被招募并整合到VIC-AJs斑块中,作为生长条件下的主要成分其特征在于增强的增殖,即在胎儿心脏瓣膜和细胞培养物中。在重新接种到脱细胞的心脏瓣膜上或在与人工支架相关的生长阶段,Pkp2在大多数情况下会从AJ中丢失。由于最近在心脏粘液瘤和其他多种间充质肿瘤的AJ中也检测到Pkp2,因此与ECM支架重新结合后,已证实的Pkp2阴性状态恢复正常,并且脱细胞的心脏瓣膜现在可为使用培养的心电图提供安全的基础瓣膜置换手术中的VIC。更令人惊讶的是,在不同类型的心内膜内皮细胞中也观察到了这种类型的Pkp2瞬时捕获,在这种情况下,它似乎与准备好进行内皮间质转化(EMT)的细胞类型相对应。

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