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首页> 外文期刊>Stem Cells >Therapeutic Effect of Human Adipose Tissue-Derived Mesenchymal Stem Cells in Experimental Corneal Failure Due to Limbal Stem Cell Niche Damage
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Therapeutic Effect of Human Adipose Tissue-Derived Mesenchymal Stem Cells in Experimental Corneal Failure Due to Limbal Stem Cell Niche Damage

机译:人类脂肪组织衍生间充质干细胞在实验角膜损伤中的治疗效果导致止血杆菌菌损伤

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Limbal stem cells are responsible for the continuous renewal of the corneal epithelium. The destruction or dysfunction of these stem cells or their niche induces limbal stem cell deficiency (LSCD) leading to visual loss, chronic pain, and inflammation of the ocular surface. To restore the ocular surface in cases of bilateral LSCD, an extraocular source of stem cells is needed to avoid dependence on allogeneic limbal stem cells that are difficult to obtain, isolate, and culture. The aim of this work was to test the tolerance and the efficacy of human adipose tissue-derived mesenchymal stem cells (hAT-MSCs) to regenerate the ocular surface in two experimental models of LSCD that closely resemble different severity grades of the human pathology. hAT-MSCs transplanted to the ocular surface of the partial and total LSCD models developed in rabbits were well tolerated, migrated to inflamed tissues, reduced inflammation, and restrained the evolution of corneal neovascularization and corneal opacity. The expression profile of the corneal epithelial cell markers CK3 and E-cadherin, and the limbal epithelial cell markers CK15 and p63 was lost in the LSCD models, but was partially recovered after hAT-MSC transplantation. For the first time, we demonstrated that hAT-MSCs improve corneal and limbal epithelial phenotypes in animal LSCD models. These results support the potential use of hAT-MSCs as a novel treatment of ocular surface failure due to LSCD. hAT-MSCs represent an available, non-immunogenic source of stem cells that may provide therapeutic benefits in addition to reduce health care expenses.
机译:恒星干细胞负责角膜上皮的连续更新。这些干细胞或其Niche的破坏或功能障碍诱导止血性干细胞缺乏(LSCD),导致眼表面的视觉损失,慢性疼痛和炎症。为了在双侧LSCD的情况下恢复眼表面,需要一种难以获得,分离和培养的同种异体突钙细胞的难以依赖性干细胞源。这项工作的目的是测试人脂肪组织衍生的间充质干细胞(HAT-MSCs)的耐受性和疗效,以在LSCD的两种实验模型中再生眼表面,其与人类病理学的不同严重程度相似。移植到兔子中开发的部分和总LSCD模型的眼表面移植的帽子MSC被耐受良好,迁移到发炎组织,降低炎症,并限制了角膜新血管形成和角膜不透明度的演变。在LSCD模型中,角膜上皮细胞标记物CK3和E-CDADHERIN的表达谱和斜纹上皮细胞标志物CK15和P63丢失,但在帽MSC移植后部分回收。我们首次证明帽子-MSCs在动物LSCD模型中改善角膜和吊顶上皮表型。这些结果支持戴帽MSCs的潜在用途作为LSCD引起的新型眼表面失效的新颖。帽子MSCs代表可提供的无可免疫原干细胞源,除了降低医疗费用外,还可以提供治疗益处。

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