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首页> 外文期刊>Biomaterials Science >The role of Sox9 in collagen hydrogel-mediated chondrogenic differentiation of adult mesenchymal stem cells (MSCs)
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The role of Sox9 in collagen hydrogel-mediated chondrogenic differentiation of adult mesenchymal stem cells (MSCs)

机译:SOX9在胶原蛋白水凝胶介导的成人间充质干细胞介导的软骨外分化的作用(MSCs)

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摘要

Sox9 is a transcription factor that regulates chondrogenesis, but its role in the chondrogenic differentiation of mesenchymal stem cells (MSCs) triggered by materials is poorly understood. In this study, we investigated the effect of Sox9 interference on collagen-induced chondrogenesis and further collagen-based therapies for cartilage defects. In this paper, MSCs were infected with a vector carrying the Sox9 promoter and related markers were detected. A lentivirus-mediated vector targeting the silencing of the Sox9 gene was used in bone marrow-derived MSCs prior to being encapsulated in a collagen hydrogel. The collagen hydrogel as a sole inducer was also compared with transforming growth factor-1 (TGF-1). Before being implanted into the articular cartilage defect in rats, the cell-hydrogel pellets were cultured in vitro for 14 days. The effect of Sox9 transfection on cell proliferation was evaluated by measuring the total DNA content. Safranin-O staining and a biochemistry assay were performed to assess the synthesis and secretion of glycosaminoglycan (GAG) of MSCs. The real-time fluorescent quantitative polymerase chain reaction (RT-PCR) was performed to detect the gene expression levels of Col1a1, Col2a1, Acan and Sox9. The protein expression of collagen type II and collagen type I was analyzed by immunohistochemical analysis. Collagen alone significantly increased the luciferase activity of the Sox9 promoter, which was in parallel with the upregulation of cartilage specific markers. In vitro, the chondrogenic differentiation ability of MSCs was greatly inhibited after Sox9 interference, both in the collagen and TGF-1-induced groups. In vivo, a further study showed that cartilage regeneration was arrested by using transfected MSCs with an injectable collagen gel or induced by TGF-1. The results indicated that collagen may mediate Sox9 expression by providing a biomimetic microenvironment favoring cell condensation prior to chondrogenesis. The role of Sox9 regulation by materials is similar to that by growth factors, suggesting that well-designed scaffolds may replace growth factors in chondrogenesis. Thus, interventions targeting Sox9 may help improve articular cartilage repair.
机译:SOX9是调节软骨发生的转录因子,但其在由材料触发的间充质干细胞(MSCs)的软骨内分化中的作用是较差的。在这项研究中,我们研究了SOX9干扰对胶原蛋白诱导的软骨发生的影响以及软骨缺陷的进一步胶原疗法。在本文中,用携带SOX9启动子的载体感染MSCs,检测相关标记。靶向SOX9基因沉默的慢病毒介导的载体在骨髓衍生的MSC中使用,然后在胶原水凝胶中包封之前。将胶原蛋白水凝胶与转化生长因子-1(TGF-1)进行比较。在大鼠中植入关节软骨缺陷之前,将细胞 - 水凝胶颗粒在体外培养14天。通过测量总DNA含量评价SOX9转染对细胞增殖的影响。进行Safranin-O染色和生物化学测定以评估MSCs的糖胺聚糖(GAG)的合成和分泌。进行实时荧光定量聚合酶链反应(RT-PCR)以检测COL1A1,COL2A1,ACAN和SOX9的基因表达水平。通过免疫组织化学分析分析II型和胶原蛋白II型和胶原蛋白类型的蛋白质表达。单独的胶原蛋白显着增加了SOX9启动子的荧光素酶活性,其与软骨特异性标记的上调平行。在体外,在SOX9干扰后,MSCs的软骨性分化能力在胶原蛋白和TGF-1诱导的基团中受到大大抑制。在体内,进一步的研究表明,通过使用用注射胶原凝胶或通过TGF-1诱导的转染MSC来阻止软骨再生。结果表明,胶原蛋白可以通过在软骨发生前提供有利于细胞缩合的仿生微环境来介导SOX9表达。 SOX9通过材料调节的作用与增长因素类似,暗示精心设计的支架可以取代软骨发生中的生长因子。因此,靶向SOX9的干预可能有助于改善关节软骨修复。

著录项

  • 来源
    《Biomaterials Science》 |2018年第6期|共13页
  • 作者单位

    Guangxi Med Univ Coll Stomatol Nanning 530021 Peoples R China;

    Guangxi Med Univ Affiliated Hosp 1 Guangxi Engn Ctr Biomed Mat Tissue &

    Organ Regene Nanning 530021 Peoples R China;

    Guangxi Med Univ Affiliated Hosp 1 Guangxi Engn Ctr Biomed Mat Tissue &

    Organ Regene Nanning 530021 Peoples R China;

    Guangxi Med Univ Affiliated Hosp 1 Guangxi Engn Ctr Biomed Mat Tissue &

    Organ Regene Nanning 530021 Peoples R China;

    Guangxi Med Univ Affiliated Hosp 1 Guangxi Engn Ctr Biomed Mat Tissue &

    Organ Regene Nanning 530021 Peoples R China;

    Sichuan Univ Natl Engn Res Ctr Biomat Chengdu 610064 Sichuan Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
  • 关键词

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