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小鼠中珠蛋白转基因的年龄依赖性沉默

Age-dependent silencing of globin transgenes in the mouse.

作者信息

Robertson G, Garrick D, Wilson M, Martin D I, Whitelaw E

机构信息

Department of Biochemistry, University of Sydney, NSW, Australia.

出版信息

Nucleic Acids Res. 1996 Apr 15;24(8):1465-71. doi: 10.1093/nar/24.8.1465.

Abstract

Variegation of transgene expression, a heterocellular or mosaic pattern of expression seen in all mice in a given transgenic line, is a frequently observed but unexplained phenomenon. We have encountered variegation with globin transgenes; when lacZ expression is driven by globin control elements a proportion of erythrocytes express beta-galactosidase (beta-gal), while the remaining erythrocytes express none. The percentage of expressing cells is constant within each line (at any particular developmental stage), but varies between lines. Such variation may account for much of the line-to-line variability which has been reported in the expression of a transgene construct. We have now extended these observations by studying expression of several globin/lacZ transgenes with increasing age. Expression of beta-gal is variegated in all lines in adult mice, including those made with a beta-globin promoter and locus control region driving lacZ. The extent of variegation differs widely between lines, but in all lines there is a marked decline in the number of erythrocytes expressing beta-gal with increasing age. Progression of silencing continues long past the point at which globin switching is complete, suggesting that it is not related to this process. We observe that age-dependent silencing is most severe in high copy number animals. Increasing variegation of transgene expression with ageing of mice is likely to complicate interpretation of the developmental regulation of transgenes. We speculate that it reflects a general mechanism of epigenetic regulation.

摘要

转基因表达的斑驳现象,即在给定转基因品系的所有小鼠中观察到的异细胞或镶嵌式表达模式,是一种经常出现但无法解释的现象。我们在珠蛋白转基因中遇到过斑驳现象;当由珠蛋白控制元件驱动lacZ表达时,一部分红细胞表达β-半乳糖苷酶(β-gal),而其余红细胞则不表达。每个品系中(在任何特定发育阶段)表达细胞的百分比是恒定的,但不同品系之间存在差异。这种差异可能解释了在转基因构建体表达中所报道的许多品系间变异性。我们现在通过研究几种珠蛋白/lacZ转基因随年龄增长的表达情况扩展了这些观察结果。在成年小鼠的所有品系中,β-gal的表达都是斑驳的,包括那些用β-珠蛋白启动子和位点控制区驱动lacZ构建的品系。不同品系间斑驳程度差异很大,但在所有品系中,随着年龄增长,表达β-gal的红细胞数量都有明显下降。沉默的进展在珠蛋白转换完成后很长时间仍在继续,这表明它与该过程无关。我们观察到,在高拷贝数动物中,年龄依赖性沉默最为严重。随着小鼠年龄增长,转基因表达的斑驳现象加剧可能会使对转基因发育调控的解释变得复杂。我们推测这反映了一种表观遗传调控的普遍机制。

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