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骨骼肌顺式调控模块预测的验证揭示了功能增强子中核苷酸组成的偏倚。

Validation of skeletal muscle cis-regulatory module predictions reveals nucleotide composition bias in functional enhancers.

机构信息

Centre for Molecular Medicine and Therapeutics, Child and Family Research Institute, Genetics Graduate Program, and Department of Medical Genetics, University of British Columbia, Vancouver, British Columbia, Canada.

出版信息

PLoS Comput Biol. 2011 Dec;7(12):e1002256. doi: 10.1371/journal.pcbi.1002256. Epub 2011 Dec 1.

Abstract

We performed a genome-wide scan for muscle-specific cis-regulatory modules (CRMs) using three computational prediction programs. Based on the predictions, 339 candidate CRMs were tested in cell culture with NIH3T3 fibroblasts and C2C12 myoblasts for capacity to direct selective reporter gene expression to differentiated C2C12 myotubes. A subset of 19 CRMs validated as functional in the assay. The rate of predictive success reveals striking limitations of computational regulatory sequence analysis methods for CRM discovery. Motif-based methods performed no better than predictions based only on sequence conservation. Analysis of the properties of the functional sequences relative to inactive sequences identifies nucleotide sequence composition can be an important characteristic to incorporate in future methods for improved predictive specificity. Muscle-related TFBSs predicted within the functional sequences display greater sequence conservation than non-TFBS flanking regions. Comparison with recent MyoD and histone modification ChIP-Seq data supports the validity of the functional regions.

摘要

我们使用三个计算预测程序对肌肉特异性顺式调控模块(CRM)进行了全基因组扫描。基于这些预测,我们在细胞培养中用 NIH3T3 成纤维细胞和 C2C12 成肌细胞对 339 个候选 CRM 进行了测试,以确定其是否有能力将选择性报告基因表达导向分化的 C2C12 肌管。验证为该测定有效的 CRM 的子集为 19 个。预测成功率表明,计算调控序列分析方法在 CRM 发现方面存在明显的局限性。基于基序的方法并不比仅基于序列保守性的预测更好。相对于无活性序列分析功能序列的特性,可以确定核苷酸序列组成是未来提高预测特异性的重要特征。在功能序列内预测的与肌肉相关的 TFBS 比非 TFBS 侧翼区域具有更高的序列保守性。与最近的 MyoD 和组蛋白修饰 ChIP-Seq 数据的比较支持功能区域的有效性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/94be/3228787/c0f3fd3208f4/pcbi.1002256.g001.jpg

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