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首页> 外文期刊>Investigative ophthalmology & visual science >Innervation of tissue-engineered recombinant human collagen-based corneal substitutes: a comparative in vivo confocal microscopy study.
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Innervation of tissue-engineered recombinant human collagen-based corneal substitutes: a comparative in vivo confocal microscopy study.

机译:组织工程重组人胶原基角膜替代品的神经支配:体内共聚焦显微镜比较研究。

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PURPOSE: To compare reinnervation in recombinant human collagen-based corneal substitutes with allografts during a 1-year postimplantation follow-up period in pigs. A retrospective comparison to innervation in porcine collagen-based biosynthetic grafts was also performed. METHODS: Pigs received a corneal allograft or a substitute made of either recombinant human type-I or -III collagen. In vivo confocal microscopic examination of the central cornea of surgical and untouched control eyes before surgery and at 2, 6, and 12 months after surgery was performed to quantify the number, density, and diameter of nerves at various corneal depths. RESULTS: By 12 months after surgery, the number and density of regenerated nerves in the anterior and deep anterior corneal stroma recovered to preoperative and control levels in both types of substitute grafts and in the allografts. In the subepithelial and subbasal regions, however, significantly fewer nerves were detected relative to those in control subjects at 12 months, regardless of graft type (P < 0.05), similar to the behavior of porcine collagen-based biosynthetic grafts. An absence of thick stromal nerve trunks (diameter, >10 mum) in all grafts, irrespective of material type, indicated that nerve regeneration in grafts was accompanied by persistent morphologic changes. CONCLUSIONS: Nerve regeneration in recombinant human collagen-based biosynthetic corneal grafts proceeded similarly to that in allograft tissue, demonstrating the suitability of recombinant human collagen constructs as nerve-friendly corneal substitutes. Furthermore, only minor differences were noted between type-I and -III collagen grafts, indicating an insensitivity of nerve regeneration to initial collagen type.
机译:目的:比较在猪植入后1年的随访期内,将同种异体移植物与重组人胶原基角膜替代品的神经支配情况。还对猪胶原蛋白基生物合成移植物中的神经支配进行了回顾性比较。方法:猪接受角膜同种异体移植物或由重组人I型或-III型胶原制成的替代物。在手术前和手术后第2、6和12个月,对手术和未接触对照眼的中央角膜进行体内共聚焦显微镜检查,以量化各种角膜深度的神经的数量,密度和直径。结果:到术后12个月,两种类型的替代移植物和同种异体移植物中,前角膜和深前角膜基质中再生神经的数量和密度均恢复到术前和对照水平。但是,在上皮下和基底下区域,与第12个月的对照组相比,无论移植类型如何(P <0.05),与对照组相比,神经的数量明显减少,这与基于猪胶原蛋白的生物合成移植物的行为相似。不论材料类型如何,所有移植物中均不存在较厚的基质神经干(直径大于10毫米),这表明移植物中的神经再生伴有持续的形态学改变。结论:基于重组人胶原蛋白的生物合成角膜移植物中的神经再生与异体移植组织中的再生相似,证明了重组人胶原蛋白结构作为神经友好性角膜替代物的适用性。此外,在I型和-III型胶原移植物之间仅观察到细微差别,表明神经再生对初始胶原类型不敏感。

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