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Comparison of the theoretical and real-world evolutionary potential of a genetic circuit

机译:遗传电路的理论和现实进化潜力的比较

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With the development of next-generation sequencing technologies, many large scale experimental efforts aim to map genotypic variability among individuals. This natural variability in populations fuels many fundamental biological processes, ranging from evolutionary adaptation and speciation to the spread of genetic diseases and drug resistance. An interesting and important component of this variability is present within the regulatory regions of genes. As these regions evolve, accumulated mutations lead to modulation of gene expression, which may have consequences for the phenotype. A simple model system where the link between genetic variability, gene regulation and function can be studied in detail is missing. In this article we develop a model to explore how the sequence of the wild-type lac promoter dictates the fold-change in gene expression. The model combines single-base pair resolution maps of transcription factor and RNA polymerase binding energies with a comprehensive thermodynamic model of gene regulation. The model was validated by predicting and then measuring the variability of lac operon regulation in a collection of natural isolates. We then implement the model to analyze the sensitivity of the promoter sequence to the regulatory output, and predict the potential for regulation to evolve due to point mutations in the promoter region.
机译:随着下一代测序技术的发展,许多大规模的实验工作旨在绘制个体之间的基因型变异性。人口的这种自然变化推动了许多基本的生物学过程,从进化适应和物种形成到遗传疾病和耐药性的传播。这种可变性的有趣且重要的组成部分存在于基因的调节区域内。随着这些区域的发展,积累的突变导致基因表达的调节,这可能对表型产生影响。缺少一个简单的模型系统,可以详细研究遗传变异性,基因调控和功能之间的联系。在本文中,我们开发了一个模型,以探索野生型lac启动子的序列如何决定基因表达的倍数变化。该模型将转录因子和RNA聚合酶结合能的单碱基对分辨率图与基因调控的综合热力学模型结合在一起。通过预测然后测量天然分离物集合中lac操纵子调控的变异性来验证该模型。然后,我们实施该模型以分析启动子序列对调节输出的敏感性,并预测由于启动子区域中的点突变而导致调节发展的潜力。

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