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通过移植基因修饰的自体表皮移植物纠正犬营养不良性大疱性表皮松解症。

Correction of dog dystrophic epidermolysis bullosa by transplantation of genetically modified epidermal autografts.

机构信息

INSERM, U634, Nice, France.

出版信息

J Invest Dermatol. 2011 Oct;131(10):2069-78. doi: 10.1038/jid.2011.172. Epub 2011 Jun 23.

Abstract

Recessive dystrophic epidermolysis bullosa (RDEB) is a severe skin blistering condition caused by mutations in the gene coding for collagen type VII. Genetically engineered RDEB dog keratinocytes were used to generate autologous epidermal sheets subsequently grafted on two RDEB dogs carrying a homozygous missense mutation in the col7a1 gene and expressing baseline amounts of the aberrant protein. Transplanted cells regenerated a differentiated and vascularized auto-renewing epidermis progressively repopulated by dendritic cells and melanocytes. No adverse immune reaction was detected in either dog. In dog 1, the grafted epidermis firmly adhered to the dermis throughout the 24-month follow-up, which correlated with efficient transduction (100%) of highly clonogenic epithelial cells and sustained transgene expression. In dog 2, less efficient (65%) transduction of primary keratinocytes resulted in a loss of the transplanted epidermis and graft blistering 5 months after transplantation. These data provide the proof of principle for ex vivo gene therapy of RDEB patients with missense mutations in collagen type VII by engraftment of the reconstructed epidermis, and demonstrate that highly efficient transduction of epidermal stem cells is crucial for successful gene therapy of inherited skin diseases in which correction of the genetic defect confers no major selective advantage in cell culture.

摘要

隐性营养不良型大疱性表皮松解症(RDEB)是一种严重的皮肤水疱病,由编码 VII 型胶原的基因突变引起。使用基因工程 RDEB 犬角朊细胞生成随后移植到携带 col7a1 基因纯合错义突变并表达基线量异常蛋白的两只 RDEB 犬上的自体表皮片。移植细胞再生出逐渐由树突状细胞和黑素细胞重新填充的分化和血管化的自我更新表皮。在这两只犬中均未检测到任何免疫反应。在犬 1 中,移植的表皮在整个 24 个月的随访过程中牢固地附着于真皮,这与高效转导(100%)高度克隆形成上皮细胞和持续的转基因表达相关。在犬 2 中,原发性角朊细胞的转导效率较低(65%)导致移植的表皮丧失,移植后 5 个月出现移植物水疱。这些数据为通过重建的表皮移植对 VII 型胶原中存在错义突变的 RDEB 患者进行体外基因治疗提供了原理证明,并表明表皮干细胞的高效转导对于遗传性皮肤病的成功基因治疗至关重要,在这些疾病中,基因缺陷的纠正在细胞培养中没有带来主要的选择性优势。

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