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Towards embryonic-like scaffolds for skin tissue engineering: identification of effector molecules and construction of scaffolds

机译:面向皮肤组织工程的类胚胎支架:效应分子的鉴定和支架的构建

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Autologous skin grafts are the gold standard for the treatment of burn wounds. In a number of cases, treatment with autologous tissue is not possible and skin substitutes are used. The outcome, however, is not optimal and improvements are needed. Inspired by scarless healing in early embryonic development, we here set out a strategy for the design and construction of embryonic-like scaffolds for skin tissue engineering. This strategy may serve as a general approach in the construction of embryonic-like scaffolds for other tissues/organ. As a first step, key effector molecules upregulated during embryonic and neonatal skin formation were identified using a comparative gene expressing analysis. A set of 20 effector molecules was identified, from which insulin-like growth factor 2 (IGF2) and sonic hedgehog (SHH) were selected for incorporation into a type I collagen-heparin scaffold. Porous scaffolds were constructed using purified collagen fibrils and 6% covalently bound heparin (to bind and protect the growth factors), and IGF2 and SHH were incorporated either individually (similar to 0.7 and 0.4 mu g/mg scaffolds) or in combination (combined similar to 1.5 mu g/mg scaffolds). In addition, scaffolds containing hyaluronan (up to 20 mu g/mg scaffold) were prepared, based on the up- or downregulation of genes involved in hyaluronan synthesis/degradation and its suggested role in scarless healing. In conclusion, based on a comprehensive gene expression analysis, a set of effector molecules and matrix molecules was identified and incorporated into porous scaffolds. The scaffolds thus prepared may create an 'embryonic-like' environment for cells to recapitulate embryonic events and for new tissues/organs. Copyright (c) 2013 John Wiley & Sons, Ltd.
机译:自体皮肤移植是烧伤创面的金标准。在许多情况下,无法用自体组织进行治疗,而是使用皮肤替代品。但是,结果并不是最佳的,需要改进。受早期胚胎发育过程中无疤愈合的启发,我们在此提出了一种设计和构建皮肤组织工程用的胚胎样支架的策略。该策略可以用作构建用于其他组织/器官的类胚胎支架的一般方法。第一步,使用比较基因表达分析鉴定在胚胎和新生儿皮肤形成过程中上调的关键效应分子。鉴定出一组20个效应分子,从中选择了胰岛素样生长因子2(IGF2)和声波刺猬(SHH)掺入I型胶原-肝素支架中。使用纯化的胶原蛋白原纤维和6%共价结合的肝素(结合并保护生长因子)构建多孔支架,IGF2和SHH可单独(类似于0.7和0.4μg / mg支架)或组合(组合类似)结合使用至1.5μg / mg支架)。此外,基于涉及透明质酸合成/降解的基因的上调或下调及其在无疤痕愈合中的作用,制备了含有透明质酸的支架(最高20μg / mg支架)。总之,基于全面的基因表达分析,鉴定了一组效应分子和基质分子,并将其整合到多孔支架中。如此制备的支架可以为细胞提供“类胚胎”环境以概括胚胎事件和新组织/器官。版权所有(c)2013 John Wiley&Sons,Ltd.

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