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首页> 外文期刊>Nucleic Acids Research >Identification of regulatory targets of tissue-specific transcription factors: application to retina-specific gene regulation
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Identification of regulatory targets of tissue-specific transcription factors: application to retina-specific gene regulation

机译:组织特异性转录因子调控靶标的鉴定:在视网膜特异性基因调控中的应用

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摘要

Identification of tissue-specific gene regulatory networks can yield insights into the molecular basis of a tissue's development, function and pathology. Here, we present a computational approach designed to identify potential regulatory target genes of photoreceptor cell-specific transcription factors (TFs). The approach is based on the hypothesis that genes related to the retina in terms of expression, disease and/or function are more likely to be the targets of retina-specific TFs than other genes. A list of genes that are preferentially expressed in retina was obtained by integrating expressed sequence tag, SAGE and microarray datasets. The regulatory targets of retina-specific TFs are enriched in this set of retina-related genes. A Bayesian approach was employed to integrate information about binding site location relative to a gene's transcription start site. Our method was applied to three retina-specific TFs, CRX, NRL and NR2E3, and a number of potential targets were predicted. To experimentally assess the validity of the bioinformatic predictions, mobility shift, transient transfection and chromatin immunoprecipitation assays were performed with five predicted CRX targets, and the results were suggestive of CRX regulation in 5/5, 3/5 and 4/5 cases, respectively. Together, these experiments strongly suggest that RP1, GUCY2D, ABCA4 are novel targets of CRX.
机译:组织特异性基因调控网络的鉴定可以深入了解组织发育,功能和病理的分子基础。在这里,我们提出了一种计算方法,旨在识别感光细胞特异性转录因子(TFs)的潜在调控靶基因。该方法基于这样的假设:就表达,疾病和/或功能而言,与视网膜相关的基因比其他基因更可能是视网膜特异性TF的靶标。通过整合表达的序列标签,SAGE和微阵列数据集,获得了在视网膜中优先表达的基因列表。视网膜特异性TF的调控靶点在这组视网膜相关基因中得到了丰富。贝叶斯方法用于整合有关结合位点相对于基因转录起始位点的信息。我们的方法应用于三个视网膜特定的TF,CRX,NRL和NR2E3,并预测了许多潜在的目标。为了通过实验评估生物信息学预测的有效性,对五个预测的CRX靶标进行了迁移率迁移,瞬时转染和染色质免疫沉淀测定,结果提示分别对5 / 5、3 / 5和4/5病例进行CRX调节。总之,这些实验强烈表明RP1,GUCY2D,ABCA4是CRX的新型靶标。

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