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Regions outside the DNA-binding domain are critical for proper in vivo specificity of an archetypal zinc finger transcription factor

机译:DNA结合结构域之外的区域对于原型锌指转录因子的正确体内特异性至关重要

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摘要

Transcription factors (TFs) are often regarded as being composed of a DNA-binding domain (DBD) and a functional domain. The two domains are considered separable and autonomous, with the DBD directing the factor to its target genes and the functional domain imparting transcriptional regulation. We examined an archetypal zinc finger (ZF) TF, Krüppel-like factor 3 with an N-terminal domain that binds the corepressor CtBP and a DBD composed of three ZFs at its C-terminus. We established a system to compare the genomic occupancy profile of wild-type Krüppel-like factor 3 with two mutants affecting the N-terminal functional domain: a mutant unable to contact the cofactor CtBP and a mutant lacking the entire N-terminal domain, but retaining the ZFs intact. Chromatin immunoprecipitation followed by sequencing was used to assess binding across the genome in murine embryonic fibroblasts. Unexpectedly, we observe that mutations in the N-terminal domain generally reduced binding, but there were also instances where binding was retained or even increased. These results provide a clear demonstration that the correct localization of TFs to their target genes is not solely dependent on their DNA-contact domains. This informs our understanding of how TFs operate and is of relevance to the design of artificial ZF proteins.
机译:转录因子(TFs)通常被认为是由DNA结合域(DBD)和功能域组成。这两个结构域被认为是可分离和自治的,DBD将因子导向其靶基因,而功能域则赋予转录调控。我们检查了原型锌指(ZF)TF,Krüppel样因子3,其N端结构域结合了心脏加压因子CtBP和在其C端由三个ZF组成的DBD。我们建立了一个系统,比较野生型Krüppel样因子3与两个影响N末端功能域的突变体的基因组占有情况:一个不能与辅因子CtBP接触的突变体和一个缺少整个N末端域的突变体,但是保留ZF完整。染色质免疫沉淀后再测序用于评估鼠胚胎成纤维细胞中整个基因组的结合。出乎意料的是,我们观察到N末端结构域中的突变通常会降低结合,但也有结合被保留甚至增加的情况。这些结果清楚地表明,TFs正确定位于其靶基因并不仅仅取决于其DNA接触域。这使我们对TF的运作方式有所了解,并且与人工ZF蛋白的设计有关。

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