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远距离作用的人类增强子的功能自主性

Functional autonomy of distant-acting human enhancers.

作者信息

Visel Axel, Akiyama Jennifer A, Shoukry Malak, Afzal Veena, Rubin Edward M, Pennacchio Len A

机构信息

Genomics Division, MS 84-171, Lawrence Berkeley National Laboratory, Berkeley, CA 94720 USA.

出版信息

Genomics. 2009 Jun;93(6):509-13. doi: 10.1016/j.ygeno.2009.02.002. Epub 2009 Mar 5.

Abstract

Many human genes are associated with dispersed arrays of transcriptional enhancers that regulate their expression in time and space. Studies in invertebrate model systems have suggested that these elements could function as discrete and independent regulatory units, but the in vivo combinatorial properties of vertebrate enhancers remain poorly understood. To explore the modularity and regulatory autonomy of human developmental enhancers, we experimentally concatenated up to four enhancers from different genes and used a transgenic mouse assay to compare the in vivo activity of these compound elements with that of the single modules. In all of the six different combinations of elements tested, the reporter gene activity patterns were additive without signs of interference between the individual modules, indicating that regulatory specificity was maintained despite the presence of closely-positioned heterologous enhancers. Even in cases where two elements drove expression in close anatomical proximity, such as within neighboring subregions of the developing limb bud, the compound patterns did not show signs of cross-inhibition between individual elements or novel expression sites. These data indicate that human developmental enhancers are highly modular and functionally autonomous and suggest that genomic enhancer shuffling may have contributed to the evolution of complex gene expression patterns in vertebrates.

摘要

许多人类基因与转录增强子的分散阵列相关联,这些增强子在时间和空间上调节基因的表达。对无脊椎动物模型系统的研究表明,这些元件可能作为离散且独立的调控单元发挥作用,但脊椎动物增强子的体内组合特性仍知之甚少。为了探索人类发育增强子的模块化和调控自主性,我们通过实验将来自不同基因的多达四个增强子串联在一起,并使用转基因小鼠试验来比较这些复合元件与单个模块在体内的活性。在测试的所有六种不同元件组合中,报告基因活性模式是相加的,各个模块之间没有干扰迹象,这表明尽管存在紧密相邻的异源增强子,调控特异性仍得以维持。即使在两个元件在解剖学上紧密相邻驱动表达的情况下,比如在发育中的肢芽的相邻子区域内,复合模式也没有显示出单个元件之间的交叉抑制迹象或新的表达位点。这些数据表明人类发育增强子具有高度模块化和功能自主性,并表明基因组增强子重排可能有助于脊椎动物复杂基因表达模式的进化。

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