首页> 外文期刊>Tissue engineering, Part C. Methods >Human primary articular chondrocytes, chondroblasts-like cells, and dedifferentiated chondrocytes: differences in gene, microRNA, and protein expression and phenotype.
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Human primary articular chondrocytes, chondroblasts-like cells, and dedifferentiated chondrocytes: differences in gene, microRNA, and protein expression and phenotype.

机译:人原发性软骨细胞,软骨母细胞样细胞和去分化软骨细胞:基因,microRNA,蛋白质表达和表型的差异。

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In this study we have isolated human primary uncultured articular chondrocytes. When these cells are allowed to proliferate within their own extracellular matrix (ECM), they begin to produce hyaline ECM molecules similar to embryological chondroblasts. These cells are called chondroblast-like cells. Upon continued culture these cells spread onto the plastic surface and dedifferentiate. We have characterized these three stages of chondral cells by gene expression and expression of microRNAs (miRNAs) and proteins. Gene expression was quantified by real-time reverse transcriptase (RT) polymerase chain reaction, miRNA expression by miRNA arrays, and protein synthesis by extra- and intracellular flow cytometry. Many of the genes, miRNAs, and proteins were differentially expressed in the different stages of chondral cells. In the context of cellular therapy, expression of some genes is a cause for concern. The best source of cells for treatment of lesions of hyaline cartilage has not yet been identified. Adult chondroblast-like cells may be strong candidates. Profound understanding of how expression of genes and synthesis of proteins are regulated in these cells, for instance, by miRNAs, may reveal new strategies for improving their synthesis of hyaline ECM. This insight is important to be able to use these cells in the clinic.
机译:在这项研究中,我们分离了人类原代未培养的关节软骨细胞。当这些细胞在其自身的细胞外基质(ECM)中增殖时,它们开始产生类似于胚胎软骨细胞的透明ECM分子。这些细胞被称为软骨母细胞样细胞。继续培养后,这些细胞扩散到塑料表面并去分化。我们已经通过基因表达以及microRNA(miRNA)和蛋白质的表达来表征这三个阶段的软骨细胞。通过实时逆转录酶(RT)聚合酶链反应,通过miRNA阵列进行miRNA表达以及通过细胞外和细胞内流式细胞术进行蛋白质合成来定量基因表达。许多基因,miRNA和蛋白质在软骨细胞的不同阶段差异表达。在细胞疗法的背景下,一些基因的表达引起关注。尚未找到治疗透明软骨损伤的最佳细胞来源。成年软骨样细胞可能是强候选者。对这些细胞中基因表达和蛋白质合成的调控方式的深刻理解,例如通过miRNA,可能揭示出改善其透明质ECM合成的新策略。这种见识对于能够在临床中使用这些细胞非常重要。

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