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Corneal Epithelial–Stromal Fibroblast Constructs to Study Cell–Cell Communication in Vitro

机译:角膜上皮 - 基质成纤维细胞体外研究细胞 - 细胞通信的构建体

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摘要

Cell–cell communication plays a fundamental role in mediating corneal wound healing following injury or infection. Depending on the severity of the wound, regeneration of the cornea and the propensity for scar development are influenced by the acute resolution of the pro-fibrotic response mediated by closure of the wound via cellular and tissue contraction. Damage of the corneal epithelium, basement membrane, and anterior stroma following a superficial keratectomy is known to lead to significant provisional matrix deposition, including secretion of fibronectin and thrombospondin-1, as well as development of a corneal scar. In addition, corneal wounding has previously been shown to promote release of extracellular vesicles from the corneal epithelium, which, in addition to soluble factors, may play a role in promoting tissue regeneration. In this study, we report the development and characterization of a co-culture system of human corneal epithelial cells and corneal stromal fibroblasts cultured for 4 weeks to allow extracellular matrix deposition and tissue maturation. The secretion of provisional matrix components, as well as small and large extracellular vesicles, was apparent within the constructs, suggesting cell–cell communication between epithelial and stromal cell populations. Laminin-1β was highly expressed by the corneal epithelial layer with the presence of notable patches of basement membrane identified by transmission electron microscopy. Interestingly, we identified expression of collagen type III, fibronectin, and thrombospondin-1 along the epithelial–stromal interface similar to observations seen in vivo following a keratectomy, as well as expression of the myofibroblast marker, α-smooth muscle actin, within the stroma. Our results suggest that this corneal epithelial–stromal model may be useful in the study of the biochemical phenomena that occur during corneal wound healing.
机译:细胞 - 细胞通信在损伤或感染后介导角膜伤口愈合中起着基本作用。取决于伤口的严重程度,角膜的再生和瘢痕发育的倾向受到通过细胞和组织收缩的伤口闭合介导的前纤维化反应的急性分辨率的影响。已知浅表角膜切除术后角膜上皮,基底膜和前基质的损伤导致显着的临时基质沉积,包括纤连蛋白和血小板运动蛋白-1的分泌,以及角膜瘢痕的发育。此外,角膜创伤先前已经显示出促进从角膜上皮,其中,除了可溶性因子,可以在促进组织再生作用的胞外囊泡的释放。在本研究中,我们报告了培养4周的人角膜上皮细胞和角膜基质成纤维细胞的共同培养系统的开发和表征,以允许细胞外基质沉积和组织成熟。在构建体中,临时基质组分以及小和大细胞外囊泡的分泌是显而易见的,表明上皮和基质细胞群之间的细胞 - 细胞连通。角膜上皮层的膜质蛋白-1β具有高度表达,并且存在通过透射电子显微镜鉴定的底部膜的显着斑块的存在。有趣的是,我们鉴定了胶原III型,纤维菌蛋白和血压素-1的表达,其上皮 - 基质界面类似于在角膜切除术后在体内观察的观察结果,以及在基质中的肌纤维细胞标记物,α-平滑肌肌动蛋白的表达。我们的研究结果表明,这种角膜上皮 - 基质模型可用于研究在角膜伤口愈合期间发生的生化现象。

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