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利用角蛋白启动子驱动生长激素转基因的转基因研究:基因治疗的前景。

Transgenic studies with a keratin promoter-driven growth hormone transgene: prospects for gene therapy.

作者信息

Wang X, Zinkel S, Polonsky K, Fuchs E

机构信息

Howard Hughes Medical Institute, Department of Molecular Genetics, The University of Chicago, IL 60637, USA.

出版信息

Proc Natl Acad Sci U S A. 1997 Jan 7;94(1):219-26. doi: 10.1073/pnas.94.1.219.

Abstract

Keratinocytes are potentially appealing vehicles for the delivery of secreted gene products because they can be transferred to human skin by the relatively simple procedure of grafting. Adult human keratinocytes can be efficiently propagated in culture with sufficient proliferative capacity to produce enough epidermis to cover the body surface of an average adult. However, the feasibility of delivering secreted proteins through skin grafting rests upon (i) the strength of the promoter in keratinocytes and (ii) the efficiency of protein transport through the basement membrane of the stratified epithelium and into the bloodstream. In this paper, we use transgenic technology to demonstrate that the activity of the human keratin 14 promoter remains high in adult skin and that keratinocyte-derived human growth hormone (hGH) can be produced, secreted, and transported to the bloodstream of mice with efficiency that is sufficient to exceed by an order of magnitude the circulating hGH concentration in growing children. Transgenic skin grafts from these adults continue to produce and secrete hGH stably, at approximately 1/10 physiological levels in the bloodstream of nontransgenic recipient mice. These studies underscore the utility of the keratin 14 promoter for expressing foreign transgenes in keratinocytes and demonstrate that keratinocytes can be used as effective vehicles for transporting factors to the bloodstream and for eliciting metabolic changes. These findings have important implications for considering the keratinocyte as a possible vehicle for gene therapy.

摘要

角质形成细胞是分泌性基因产物递送的潜在理想载体,因为它们可以通过相对简单的移植程序转移到人体皮肤。成人角质形成细胞能够在培养中高效增殖,具有足够的增殖能力以产生足够覆盖普通成年人身体表面的表皮。然而,通过皮肤移植递送分泌蛋白的可行性取决于:(i)角质形成细胞中启动子的强度;(ii)蛋白质通过复层上皮基底膜并进入血液循环的效率。在本文中,我们利用转基因技术证明人角蛋白14启动子在成人皮肤中活性仍然很高,并且角质形成细胞来源的人生长激素(hGH)能够产生、分泌并运输到小鼠血液中,其效率足以比生长中儿童的循环hGH浓度高出一个数量级。来自这些成年人的转基因皮肤移植物继续稳定地产生和分泌hGH,在非转基因受体小鼠血液中的水平约为生理水平的1/10。这些研究强调了角蛋白14启动子在角质形成细胞中表达外源转基因的实用性,并证明角质形成细胞可作为将因子运输到血液中并引发代谢变化的有效载体。这些发现对于将角质形成细胞视为基因治疗的可能载体具有重要意义。

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