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Porcine Fetal-Derived Fibroblasts Alter Gene Expression and Mitochondria to Compensate for Hypoxic Stress During Culture

机译:猪胎儿成纤维细胞改变基因表达和线粒体以补偿培养过程中的低氧应激

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摘要

The Warburg effect is characterized by decreased mitochondrial oxidative phosphorylation and increased glycolytic flux in adequate oxygen. The preimplantation embryo has been described to have characteristics of the Warburg effect, including similar changes in gene expression and mitochondria, which are more rudimentary in appearance. We hypothesized hypoxia would facilitate anaerobic glycolysis in fibroblasts thereby promoting gene expression and media metabolite production reflecting the Warburg effect hallmarks in early embryos. Additionally, we speculated that hypoxia would induce a rudimentary small mitochondrial phenotype observed in several cell types evidenced to demonstrate the Warburg effect. While many have examined the role hypoxia plays in pathological conditions, few studies have investigated changes in primary cells which could be used in somatic cell nuclear transfer. We found that cells grown in 1.25% O2 had normal cell viability and more, but smaller mitochondria. Several hypoxia-inducible genes were identified, including seven genes for glycolytic enzymes. In conditioned media from hypoxic cells, the quantities of gluconolactone, cytosine, and uric acid were decreased indicating higher consumption than control cells. These results indicate that fibroblasts alter gene expression and mitochondria to compensate for hypoxic stress and maintain viability. Furthermore, the metabolic changes observed, making them more similar to preimplantation embryos, could be facilitating nuclear reprogramming making these cells more amendable to future use in somatic cell nuclear transfer.
机译:沃堡效应的特征在于线粒体氧化磷酸化的减少和在充足氧气中糖酵解通量的增加。已经描述了植入前的胚胎具有沃伯格效应的特征,包括基因表达和线粒体的相似变化,这些变化在外观上更为基本。我们假设缺氧会促进成纤维细胞中的厌氧糖酵解,从而促进基因表达和培养基代谢产物的产生,从而反映出早期胚胎中的Warburg效应。此外,我们推测缺氧会诱导在证明具有Warburg效应的几种细胞类型中观察到的基本线粒体表型。尽管许多人研究了缺氧在病理状况中的作用,但很少有研究研究可用于体细胞核移植的原代细胞的变化。我们发现,在1.25%的O2中生长的细胞具有正常的细胞活力,并且具有更高的线粒体活力。确定了几个缺氧诱导基因,包括糖酵解酶的七个基因。在来自缺氧细胞的条件培养基中,葡糖酸内酯,胞嘧啶和尿酸的数量减少,表明其消耗量高于对照细胞。这些结果表明,成纤维细胞改变基因表达和线粒体以补偿低氧应激并维持生存力。此外,观察到的代谢变化使它们与植入前的胚胎更相似,可能促进核重编程,使这些细胞更适合将来用于体细胞核移植。

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