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生长激素因子-1启动子靶向的促生长祖细胞永生化导致转基因小鼠出现侏儒症。

GHF-1-promoter-targeted immortalization of a somatotropic progenitor cell results in dwarfism in transgenic mice.

作者信息

Lew D, Brady H, Klausing K, Yaginuma K, Theill L E, Stauber C, Karin M, Mellon P L

机构信息

Department of Reproductive Medicine, University of California, San Diego, School of Medicine, La Jolla 92093.

出版信息

Genes Dev. 1993 Apr;7(4):683-93. doi: 10.1101/gad.7.4.683.

DOI:10.1101/gad.7.4.683
PMID:8096199
Abstract

During pituitary development, the homeo domain protein GHF-1 is required for generation of somatotropes and lactotropes and for growth hormone (GH) and prolactin (PRL) gene expression. GHF-1 mRNA is detectable several days before the emergence of GH- or PRL-expressing cells, suggesting the existence of a somatotropic progenitor cell in which GHF-1 transcription is first activated. We have immortalized this cell type by using the GHF-1 regulatory region to target SV40 T-antigen (Tag) tumorigenesis in transgenic mice. The GHF-Tag transgene caused developmental entrapment of somatotropic progenitor cells that express GHF-1 but not GH or PRL, resulting in dwarfism. Immortalized cell lines derived from a transgenic pituitary tumor maintain the characteristics of the somato/lactotropic progenitor in that they express GHF-1 mRNA and protein yet fail to activate GH or PRL transcription. Using these cells, we identified an enhancer that activates GHF-1 transcription at this early stage of development yet is inactive in cells representing later developmental stages of the somatotropic lineage or in other cell types. These experiments not only demonstrate the potential for immortalization of developmental progenitor cells using the regulatory regions from cell type-specific transcription factor genes but illustrate the power of such model systems in the study of developmental control.

摘要

在垂体发育过程中,同源结构域蛋白GHF-1对于生长激素细胞和催乳激素细胞的产生以及生长激素(GH)和催乳素(PRL)基因的表达是必需的。在表达GH或PRL的细胞出现前几天就能检测到GHF-1 mRNA,这表明存在一种生长激素祖细胞,其中GHF-1转录首先被激活。我们通过利用GHF-1调控区在转基因小鼠中靶向SV40 T抗原(Tag)致瘤作用,使这种细胞类型永生化。GHF-Tag转基因导致表达GHF-1但不表达GH或PRL的生长激素祖细胞发育停滞,从而导致侏儒症。源自转基因垂体肿瘤的永生化细胞系保持了生长激素/催乳激素祖细胞的特征,即它们表达GHF-1 mRNA和蛋白,但未能激活GH或PRL转录。利用这些细胞,我们鉴定出一种增强子,它在发育的早期阶段激活GHF-1转录,但在代表生长激素谱系后期发育阶段的细胞或其他细胞类型中无活性。这些实验不仅证明了利用细胞类型特异性转录因子基因的调控区使发育祖细胞永生化的可能性,还说明了这种模型系统在发育控制研究中的作用。

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