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皮肤基因转移与治疗:现状与未来。

Cutaneous gene transfer and therapy: the present and the future.

作者信息

Spirito F, Meneguzzi G, Danos O, Mezzina M

机构信息

INSERM U385 Faculté de Médecine, Nice, France.

出版信息

J Gene Med. 2001 Jan-Feb;3(1):21-31. doi: 10.1002/1521-2254(2000)9999:9999<::AID-JGM156>3.0.CO;2-I.

DOI:10.1002/1521-2254(2000)9999:9999<::AID-JGM156>3.0.CO;2-I
PMID:11269332
Abstract

The easy accessibility of the skin as a therapeutic target provides an exciting potential for this organ for the development of gene therapy protocols for cutaneous diseases and a variety of metabolic disorders. Thus far, full phenotypic reversion of a diseased phenotype has been achieved in vivo for junctional epidermolysis bullosa and X-linked or lamellar ichthyosis and in vitro for xeroderma pigmentosum. These recessive skin diseases are characterized by skin blistering, abnormalities in epidermal differentiation and increased development of skin cancers, respectively. Corrective gene delivery at both molecular and functional levels was achieved by transduction of cultured skin cells using retroviral vectors carrying the specific curative cDNA. These positive results should prompt clinical trials based on transplantation of artificial epithelia reconstructed ex vivo using genetically modified keratinocytes. Promising results have also been obtained in phenotypic reversion of cells isolated from patients suffering from a number of metabolic diseases such as gyrate atrophy, familial hypercholesterolemia or phenylketonuria. In these diseases transplantation of autologous artificial epithelia expressing the transgenes of interest or direct transfer of the DNA to the skin represents a potential therapeutic approach for the systemic delivery of active molecules. Successful cutaneous gene therapy trials, however, require development of protocols for efficient gene transfer to epidermal stem cells, and information about the host immune response to the recombinant polypeptides produced by the implanted keratinocytes. The availability of spontaneous animal models for genodermatoses will validate the gene therapy approach in preclinical trials.

摘要

皮肤作为治疗靶点易于接触,为该器官开发用于治疗皮肤疾病和各种代谢紊乱的基因治疗方案提供了令人兴奋的潜力。迄今为止,在体内已实现交界性大疱性表皮松解症、X连锁鱼鳞病或板层状鱼鳞病患病表型的完全表型逆转,在体外已实现着色性干皮病的表型逆转。这些隐性皮肤病分别以皮肤水疱、表皮分化异常和皮肤癌发病率增加为特征。通过使用携带特定治疗性cDNA的逆转录病毒载体转导培养的皮肤细胞,在分子和功能水平上实现了纠正性基因传递。这些积极结果应促使开展基于使用基因修饰角质形成细胞体外重建人工上皮进行移植的临床试验。在从患有多种代谢疾病(如回旋状萎缩、家族性高胆固醇血症或苯丙酮尿症)的患者中分离出的细胞的表型逆转方面也取得了有希望的结果。在这些疾病中,移植表达感兴趣转基因的自体人工上皮或将DNA直接转移到皮肤代表了一种用于全身递送活性分子的潜在治疗方法。然而,成功的皮肤基因治疗试验需要开发将基因有效转移到表皮干细胞的方案,以及有关宿主对植入角质形成细胞产生的重组多肽的免疫反应的信息。遗传性皮肤病自发动物模型的可用性将在临床前试验中验证基因治疗方法。

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Corrective gene transfer of keratinocytes from patients with junctional epidermolysis bullosa restores assembly of hemidesmosomes in reconstructed epithelia.交界性大疱性表皮松解症患者角质形成细胞的矫正基因转移可恢复重建上皮中半桥粒的组装。
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Curr Gene Ther. 2016;16(2):83-9. doi: 10.2174/1566523216666160331125810.
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Topical gene electrotransfer to the epidermis of hairless guinea pig by non-invasive multielectrode array.经非侵入式多电极阵列将基因电转导入无毛豚鼠表皮。
PLoS One. 2013 Aug 28;8(8):e73423. doi: 10.1371/journal.pone.0073423. eCollection 2013.
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Nucleofection: a new method for cutaneous gene transfer?核转染:一种皮肤基因转移的新方法?
J Biomed Biotechnol. 2006;2006(5):26060. doi: 10.1155/JBB/2006/26060.
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Adenoviral gene delivery to primary human cutaneous cells and burn wounds.腺病毒介导的基因传递至原代人皮肤细胞和烧伤创面。
Mol Med. 2006 Sep-Oct;12(9-10):199-207. doi: 10.2119/2006-00031.Hirsch.