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基因表达的远程调控:新出现的机制及在疾病中的破坏

Long-range control of gene expression: emerging mechanisms and disruption in disease.

作者信息

Kleinjan Dirk A, van Heyningen Veronica

机构信息

MRC Human Genetics Unit, Western General Hospital, Crewe Road, Edinburgh EH4 2XU, Scotland, United Kingdom.

出版信息

Am J Hum Genet. 2005 Jan;76(1):8-32. doi: 10.1086/426833. Epub 2004 Nov 17.

Abstract

Transcriptional control is a major mechanism for regulating gene expression. The complex machinery required to effect this control is still emerging from functional and evolutionary analysis of genomic architecture. In addition to the promoter, many other regulatory elements are required for spatiotemporally and quantitatively correct gene expression. Enhancer and repressor elements may reside in introns or up- and downstream of the transcription unit. For some genes with highly complex expression patterns--often those that function as key developmental control genes--the cis-regulatory domain can extend long distances outside the transcription unit. Some of the earliest hints of this came from disease-associated chromosomal breaks positioned well outside the relevant gene. With the availability of wide-ranging genome sequence comparisons, strong conservation of many noncoding regions became obvious. Functional studies have shown many of these conserved sites to be transcriptional regulatory elements that sometimes reside inside unrelated neighboring genes. Such sequence-conserved elements generally harbor sites for tissue-specific DNA-binding proteins. Developmentally variable chromatin conformation can control protein access to these sites and can regulate transcription. Disruption of these finely tuned mechanisms can cause disease. Some regulatory element mutations will be associated with phenotypes distinct from any identified for coding-region mutations.

摘要

转录调控是调节基因表达的主要机制。实现这种调控所需的复杂机制仍在从基因组结构的功能和进化分析中逐渐显现。除启动子外,基因在时空和定量上的正确表达还需要许多其他调控元件。增强子和抑制元件可能位于内含子或转录单元的上下游。对于一些具有高度复杂表达模式的基因——通常是那些作为关键发育控制基因发挥作用的基因——顺式调控域可在转录单元之外延伸很长距离。对此的一些最早线索来自位于相关基因之外很远位置的与疾病相关的染色体断裂。随着广泛的基因组序列比较的出现,许多非编码区域的强烈保守性变得明显。功能研究表明,这些保守位点中的许多是转录调控元件,有时位于不相关的相邻基因内部。这种序列保守元件通常含有组织特异性DNA结合蛋白的位点。发育过程中可变的染色质构象可控制蛋白质对这些位点的访问,并可调节转录。这些精细调节机制的破坏会导致疾病。一些调控元件突变将与不同于任何已确定的编码区突变的表型相关。

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