Department of Immunobiology, UCL Institute of Child Health, London, UK.
Mol Ther. 2011 Feb;19(2):408-16. doi: 10.1038/mt.2010.201. Epub 2010 Sep 28.
Netherton syndrome (NS) is a debilitating congenital skin disorder caused by mutations in the SPINK5 gene encoding the lymphoepithelial Kazal-type-related inhibitor (LEKTI). It is characterized by defective keratinization, recurrent infections, and hypernatraemic dehydration with a mortality rate of about 10% in the first year of life. Currently, there are no curative treatments for NS. We have developed a HIV-1 based, self-inactivating lentiviral vector to express SPINK5 in keratinocytes as part of an ex-vivo gene therapy strategy for NS. High transduction efficiency was achieved in NS keratinocytes and reconstitution of LEKTI expression was confirmed in previously deficient cells. These genetically corrected keratinocytes were further tested in an in vitro organotypic culture (OTC) system and in vivo mouse/human skin engraftment model. Results showed correction of epidermal architecture in both OTCs and regenerated skin grafts. Importantly, the results from corrected skin grafts indicated that even where detectable LEKTI expression was restored to a limited numbers of cells, a wider bystander benefit occurred around these small populations. As LEKTI is a secreted protein, the genetically modified graft may provide not only an immediate local protective barrier, but also act as a source of secreted LEKTI providing a generalized benefit following ex-vivo gene therapy.
Netherton 综合征(NS)是一种由编码淋巴上皮 Kazal 型相关抑制剂(LEKTI)的 SPINK5 基因突变引起的致残性先天性皮肤疾病。其特征为角化缺陷、反复感染和高钠血症脱水,在生命的第一年死亡率约为 10%。目前,NS 尚无治愈方法。我们开发了一种基于 HIV-1 的、自失活的慢病毒载体,以在角质形成细胞中表达 SPINK5,作为 NS 体外基因治疗策略的一部分。在 NS 角质形成细胞中实现了高转导效率,并在先前缺乏 LEKTI 的细胞中证实了其表达的重建。这些经过基因修正的角质形成细胞进一步在体外器官型培养(OTC)系统和体内小鼠/人皮肤移植模型中进行了测试。结果表明,在 OTC 和再生皮肤移植物中都纠正了表皮结构。重要的是,经过修正的皮肤移植物的结果表明,即使 LEKTI 的表达在有限数量的细胞中得到了恢复,在这些小群体周围也会发生更广泛的旁观者效应。由于 LEKTI 是一种分泌蛋白,经过基因修饰的移植物不仅可以提供即时的局部保护屏障,还可以作为分泌型 LEKTI 的来源,在体外基因治疗后提供广泛的益处。