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α1(I)型胶原-hGH 微型基因在转基因小鼠中的细胞特异性表达

Cell-specific expression of alpha 1(I) collagen-hGH minigenes in transgenic mice.

作者信息

Liska D J, Reed M J, Sage E H, Bornstein P

机构信息

Department of Biochemistry, University of Washington, Seattle 98195.

出版信息

J Cell Biol. 1994 May;125(3):695-704. doi: 10.1083/jcb.125.3.695.

Abstract

Sequences within the first intron of the alpha 1(I) collagen gene have been implicated in the regulation of expression of alpha 1(I) collagen-reporter gene constructs in cultured cells. However, the physiological significance of these intronic elements has not been established. We have used in situ hybridization to examine whether a cell-specific pattern of expression of human alpha 1(I) collagen-human growth hormone minigenes exists in transgenic mice. Our results indicate that transgenes which contained 2,300 bp of promoter/5' flanking sequence and an intact first intron were well expressed by fibroblasts in dermis and fascia, whereas transgenes lacking the intronic sequence, +292 to +1440, were not expressed in dermis and poorly expressed in fascia. Analysis of transgene expression in cultured fibroblasts obtained from dermal explants of transgenic animals confirmed the requirement for these intronic sequences in the regulation of the alpha 1(I) collagen gene. In contrast, transgenes with or without the intronic deletion were expressed equally well in tendon and bone, in a manner comparable to the endogenous mouse alpha 1(I) collagen gene, and expression of neither transgene was detected in skeletal muscle or perichondrium. These data support a model in which cis-acting elements in the first intron, and their cognate DNA-binding proteins, mediate transcription of the alpha 1(I) collagen gene in some cells, such as dermal fibroblasts, but not in tendon cells or osteoblasts. Moreover, regions of the gene not included in the sequence, -2300 to +1440, appear to be required for transcription in tissues such as skeletal muscle and perichondrium.

摘要

α1(I)型胶原蛋白基因第一个内含子中的序列与培养细胞中α1(I)型胶原蛋白报告基因构建体的表达调控有关。然而,这些内含子元件的生理意义尚未确定。我们利用原位杂交技术检测转基因小鼠中是否存在人α1(I)型胶原蛋白 - 人生长激素微型基因的细胞特异性表达模式。我们的结果表明,含有2300 bp启动子/ 5'侧翼序列和完整第一个内含子的转基因在真皮和筋膜中的成纤维细胞中表达良好,而缺乏内含子序列(+292至+1440)的转基因在真皮中不表达,在筋膜中表达不佳。对从转基因动物皮肤外植体获得的培养成纤维细胞中的转基因表达分析证实了这些内含子序列对α1(I)型胶原蛋白基因调控的必要性。相比之下,有或没有内含子缺失的转基因在肌腱和骨骼中的表达同样良好,其方式与内源性小鼠α1(I)型胶原蛋白基因相当,并且在骨骼肌或软骨膜中均未检测到任何一种转基因的表达。这些数据支持了一种模型,即第一个内含子中的顺式作用元件及其同源DNA结合蛋白在某些细胞(如真皮成纤维细胞)中介导α1(I)型胶原蛋白基因的转录,但在肌腱细胞或成骨细胞中则不然。此外,基因中不包括在-2300至+1440序列中的区域似乎是骨骼肌和软骨膜等组织中转录所必需的。

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本文引用的文献

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Regulation of expression of the type I collagen genes.I型胶原蛋白基因表达的调控
Am J Med Genet. 1993 Jan 15;45(2):140-51. doi: 10.1002/ajmg.1320450203.

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