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富含调控基序的基因组区域中基因表达的出现与演变。

The emergence and evolution of gene expression in genome regions replete with regulatory motifs.

作者信息

Fuqua Timothy, Sun Yiqiao, Wagner Andreas

机构信息

Department of Evolutionary Biology and Environmental Studies, University of Zurich, Zurich, Switzerland.

Swiss Institute of Bioinformatics, Quartier Sorge-Batiment Genopode, Lausanne, Switzerland.

出版信息

Elife. 2024 Dec 20;13:RP98654. doi: 10.7554/eLife.98654.

Abstract

Gene regulation is essential for life and controlled by regulatory DNA. Mutations can modify the activity of regulatory DNA, and also create new regulatory DNA, a process called regulatory emergence. Non-regulatory and regulatory DNA contain motifs to which transcription factors may bind. In prokaryotes, gene expression requires a stretch of DNA called a promoter, which contains two motifs called -10 and -35 boxes. However, these motifs may occur in both promoters and non-promoter DNA in multiple copies. They have been implicated in some studies to improve promoter activity, and in others to repress it. Here, we ask whether the presence of such motifs in different genetic sequences influences promoter evolution and emergence. To understand whether and how promoter motifs influence promoter emergence and evolution, we start from 50 'promoter islands', DNA sequences enriched with -10 and -35 boxes. We mutagenize these starting 'parent' sequences, and measure gene expression driven by 240,000 of the resulting mutants. We find that the probability that mutations create an active promoter varies more than 200-fold, and is not correlated with the number of promoter motifs. For parent sequences without promoter activity, mutations created over 1500 new -10 and -35 boxes at unique positions in the library, but only ~0.3% of these resulted in de-novo promoter activity. Only ~13% of all -10 and -35 boxes contribute to de-novo promoter activity. For parent sequences with promoter activity, mutations created new -10 and -35 boxes in 11 specific positions that partially overlap with preexisting ones to modulate expression. We also find that -10 and -35 boxes do not repress promoter activity. Overall, our work demonstrates how promoter motifs influence promoter emergence and evolution. It has implications for predicting and understanding regulatory evolution, de novo genes, and phenotypic evolution.

摘要

基因调控对生命至关重要,且受调控性DNA控制。突变可改变调控性DNA的活性,还能创造新的调控性DNA,这一过程称为调控性涌现。非调控性DNA和调控性DNA都含有转录因子可能结合的基序。在原核生物中,基因表达需要一段称为启动子的DNA,它包含两个称为-10盒和-35盒的基序。然而,这些基序可能以多个拷贝出现在启动子和非启动子DNA中。在一些研究中,它们被认为可提高启动子活性,而在另一些研究中则被认为会抑制启动子活性。在此,我们探讨不同基因序列中此类基序的存在是否会影响启动子的进化和涌现。为了解启动子基序是否以及如何影响启动子的涌现和进化,我们从50个“启动子岛”开始,即富含-10盒和-35盒的DNA序列。我们对这些起始的“亲本”序列进行诱变,并测量由24万个所得突变体驱动的基因表达。我们发现,突变产生活性启动子的概率变化超过200倍,且与启动子基序的数量无关。对于没有启动子活性的亲本序列,突变在文库中的独特位置产生了超过1500个新的-10盒和-35盒,但其中只有约0.3%导致了从头启动子活性。所有-10盒和-35盒中只有约13%有助于从头启动子活性。对于具有启动子活性的亲本序列,突变在11个特定位置产生了新的-10盒和-35盒,这些位置与先前存在的部分重叠,以调节表达。我们还发现,-10盒和-35盒不会抑制启动子活性。总体而言,我们的工作展示了启动子基序如何影响启动子的涌现和进化。它对预测和理解调控进化、从头基因和表型进化具有启示意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4141/11661796/3b5db1359abe/elife-98654-fig2-figsupp1.jpg

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