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Tissue engineered biomimetic corneas for promoting corneal regeneration.

机译:组织工程仿生角膜,用于促进角膜再生。

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摘要

Corneal transplantation with allograft tissue is currently the gold standard treatment for treating corneal damage following trauma or disease. However the supply of good quality donor tissue cannot meet the demand, especially in developing countries. Currently, the only alternative treatment option has been the use of corneal prostheses (keratoprostheses) but these do not permit integration with the host tissue. We utilized a regenerative medicine approach to enhance the natural ability of the cornea to regenerate by providing an acellular but highly bioactive scaffold to serve as a corneal extracellular matrix (ECM) substitute. The corneal substitutes tested were based on the predominant ECM protein found in the cornea, which is type I collagen. Cross-linked collagen corneal scaffolds were formed into the appropriated dimensions and cross linked using a simple methodology, and tested in vitro to assure that they would support cellular growth of epithelial cells and nerves. The most promising candidate implants were then implanted into a range of animal models as either lamellar grafts, or full thickness grafts by lamellar and penetrating keratoplasties, respectively. Following implantation, it was observed that the scaffolds promoted regeneration of the corneal epithelial and stromal cells. The implants themselves were remodelled, observed through biotin conjugation, to give a seamless host-graft interface. The grafts remained stably integrated. At 12 months post implantation, the implanted corneas had comparable mechanical properties compared to contralateral controls. Nerves had reinnervated the cornea at densities comparable to controls and were shown to be functionally active, capable of responding to external stimuli through electrophysiological testing. We were also able to improve the mechanical properties of our gels by incorporating the biomimetic molecule 2-methacryloyloxyethyl phosphorylcholine (MPC), which allowed for full thickness transplantation into guinea pigs. Finally, with the advent of recombinant human collagen, we were able to create a novel class of human based materials for corneal implantation, which were successfully transplanted into pigs. Type III recombinant human collagen, a minor component of the human cornea, showed superior optical transmission compared to type I collagen gels, and both showed stable integration, with corneal regeneration of cells, tear film, and nerves. Substantially more work is needed to determine the limits of this approach in treating corneal blindness, i.e. what clinical causes of blindness can be treated in this manner. Nevertheless, we have demonstrated that a simple, ECM mimetic could promote the regeneration of corneal cell types, and the reinnervation of functional nerves, in a stable and seamless fashion.
机译:目前,同种异体组织的角膜移植是治疗创伤或疾病后角膜损伤的金标准治疗方法。但是,高质量供体组织的供应不能满足需求,特别是在发展中国家。当前,唯一的替代治疗选择是使用角膜假体(角膜假体),但是这些方法不允许与宿主组织整合。我们利用再生医学方法通过提供无细胞但具有高生物活性的支架作为角膜细胞外基质(ECM)替代物来增强角膜的自然再生能力。测试的角膜替代品基于在角膜中发现的主要ECM蛋白,即I型胶原蛋白。交联的胶原蛋白角膜支架形成适当的尺寸,并使用简单的方法进行交联,并在体外进行测试,以确保它们将支持上皮细胞和神经的细胞生长。然后,最有前途的候选植入物分别通过层状和穿透性角膜移植手术植入各种动物模型中,成为片状移植物或全厚度移植物。植入后,观察到支架促进角膜上皮和基质细胞的再生。通过生物素结合观察,对植入物本身进行了重塑,以提供无缝的宿主-移植物界面。移植物保持稳定整合。植入后12个月,与对侧对照相比,植入的角膜具有可比的机械性能。神经以与对照组相当的密度重新激活了角膜,并被证明具有功能活性,能够通过电生理学测试对外部刺激做出反应。通过掺入仿生分子2-甲基丙烯酰氧基乙基磷酰胆碱(MPC),我们还能够改善凝胶的机械性能,从而可以将其完全移植到豚鼠中。最后,随着重组人类胶原蛋白的出现,我们能够创建一类新型的人类角膜植入材料,并将其成功移植到猪中。与I型胶原蛋白凝胶相比,III型重组人胶原蛋白(人类角膜的次要组成部分)显示出出众的透光性,并且都显示出稳定的整合,并具有角膜再生细胞,泪膜和神经。为了确定这种方法在治疗角膜盲症中的局限性,需要大量的工作,即可以用这种方式治疗失明的临床原因。然而,我们已经证明,简单,ECM模仿物可以稳定和无缝的方式促进角膜细胞类型的再生和功能神经的重新支配。

著录项

  • 作者单位

    University of Ottawa (Canada).;

  • 授予单位 University of Ottawa (Canada).;
  • 学科 Biology Molecular.
  • 学位 Ph.D.
  • 年度 2009
  • 页码 214 p.
  • 总页数 214
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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