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Development of Orchestrated Stem Cell-based Regeneration (OSCeR) - Strategies to recruit and differentiate autologous stem cells for tissue regeneration.

机译:精心设计的基于干细胞的再生(OSCeR)的开发-招募和分化自体干细胞用于组织再生的策略。

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摘要

Stem cell therapy has shown great promise in curing diseases. However, clinical application of stem cell therapy is often hindered by the lack of reliable sources and convenient methods to recover stem cells. Our laboratory has recently discovered that adult stem cells can be actively recruited via inflammatory chemokines/growth factor. My research was aimed towards the development of a new technology - "Orchestrated Stem Cell-based Regeneration" or OSCeR - to induce stem cell-mediated tissue regeneration by blending stem cell therapy and tissue engineering technology. This work has led to a series of interesting findings as listed below.;Shortly after implantation, biomaterial implants are often accompanied by large numbers of mesenchymal stem cells (MSC) and hematopoietic stem cells (HSC) around the implantation sites. These spontaneously recruited multipotent stem cells could be differentiated into various lineages in vitro. Subsequent studies confirmed that there is a good relationship between the extent of inflammatory responses and stem cell recruitment. Very interestingly, by supplementing an osteogenic factor [bone morphogenetic protein-2 (BMP-2)] in scaffolds, the recruited multipotent stem cells turned into an osteogenic type and formed mineralized tissue in the subcutaneous soft tissue space. To apply OSCeR for regenerating different tissue, one of the main challenges was to establish scaffold a fabrication technique that could incorporate a variety of cytokines and growth factors. This was imperative since almost all tissue engineering scaffolds are unable to load and release proteins in an active form. Based on our preliminary work, we established a microbubble scaffold fabrication technique which can easily load and release bioactive proteins over a period of time. The scaffolds were characterized in an in vitro and in vivo setting.;With the microbubble scaffold technique, we investigated the feasibility of applying OSCeR technology for bone and vascular graft regeneration. For bone application, a combination of BMP and erythropoietin prompted maximal cell infiltration and showed signs of bone formation. To regenerate vascular grafts, we used an intra-peritoneal implantation model to study the vascular tissue formation, especially endothelialization, of the inner lumen of biphasic vascular grafts - crosslinked urethane doped polyester (CUPE). Within a week of SDVG implantation, the lumen was quickly covered with endothelial progenitor cells and by week 2 there were signs of endothelial cells lining the lumen.;Through these studies we were able to develop a novel OSCeR technology which turns the normally unwanted foreign body reactions into an appreciable phenomenon of in vivo tissue regeneration. The results from this work prove that, by blending stem cell therapy and tissue engineering, OSCeR technology may have a bright future in regenerative medicine.
机译:干细胞疗法在治疗疾病方面显示出巨大的希望。然而,干细胞疗法的临床应用常常由于缺乏可靠的来源和方便的回收干细胞的方法而受到阻碍。我们的实验室最近发现,成人干细胞可以通过炎症趋化因子/生长因子积极募集。我的研究旨在开发一种新技术-“基于器官的干细胞再生”或OSCeR-通过混合干细胞疗法和组织工程技术来诱导干细胞介导的组织再生。这项工作导致了一系列有趣的发现,如下所示:植入后不久,生物材料植入物通常在植入部位周围伴随着大量的间充质干细胞(MSC)和造血干细胞(HSC)。这些自发募集的多能干细胞可以在体外分化成各种谱系。随后的研究证实,炎症反应的程度与干细胞募集之间存在良好的关系。非常有趣的是,通过在支架中补充成骨因子[骨形态发生蛋白2(BMP-2)],募集的多能干细胞变成了成骨类型并在皮下软组织空间中形成了矿化的组织。为了将OSCeR应用于再生不同的组织,主要的挑战之一是建立一种可以结合多种细胞因子和生长因子的制造技术。这是必须的,因为几乎所有组织工程支架都无法以活性形式加载和释放蛋白质。基于我们的初步工作,我们建立了一种微泡支架制造技术,该技术可以在一段时间内轻松加载和释放生物活性蛋白。在体外和体内环境中对支架进行了表征。通过微泡支架技术,我们研究了将OSCeR技术应用于骨骼和血管移植物再生的可行性。对于骨应用,BMP和促红细胞生成素的组合可促进最大的细胞浸润并显示出骨形成的迹象。为了再生血管移植物,我们使用了腹膜内植入模型来研究双相血管移植物内腔-交联氨基甲酸乙酯掺杂聚酯(CUPE)的血管组织形成,特别是内皮化。在植入SDVG的一周内,内腔迅速被内皮祖细胞覆盖,到第2周时,内腔内壁出现了内皮细胞的迹象。通过这些研究,我们得以开发出一种新颖的OSCeR技术,该技术可以转变通常不需要的异物反应变成体内组织再生的明显现象。这项工作的结果证明,通过将干细胞疗法与组织工程技术相结合,OSCeR技术在再生医学中可能具有光明的前景。

著录项

  • 作者

    Nair, Ashwin.;

  • 作者单位

    The University of Texas at Arlington.;

  • 授予单位 The University of Texas at Arlington.;
  • 学科 Biology Cell.;Engineering Biomedical.
  • 学位 Ph.D.
  • 年度 2010
  • 页码 113 p.
  • 总页数 113
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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