Transcriptome profiling of maize transcription factor mutants to probe gene regulatory network predictions.

IF 2.1 3区 生物学 Q3 GENETICS & HEREDITY
Erika L Ellison, Peng Zhou, Yi-Hsuan Chu, Peter Hermanson, Lina Gomez-Cano, Zachary A Myers, Ankita Abnave, John Gray, Candice N Hirsch, Erich Grotewold, Nathan M Springer
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Abstract

Transcription factors (TFs) play important roles in regulation of gene expression and phenotype. A variety of approaches have been utilized to develop gene-regulatory networks (GRNs) to predict the regulatory targets for each TF, such as yeast-one-hybrid (Y1H) screens and gene co-expression network (GCN) analysis. Here we identified potential TF targets and used a reverse genetics approach to test the predictions of several GRNs in maize. Loss-of-function mutant alleles were isolated for 22 maize TFs. These mutants did not exhibit obvious morphological phenotypes. However, transcriptomic profiling identified differentially expressed genes in each of the mutant genotypes, and targeted metabolic profiling indicated variable phenolic accumulation in some mutants. An analysis of expression levels for predicted target genes based on Y1H screens identified a small subset of predicted targets that exhibit altered expression levels. The analysis of predicted targets from GCN-based methods found significant enrichments for prediction sets of some TFs, but most predicted targets did not exhibit altered expression. This could result from false-positive GCN predictions, a TF with a secondary regulatory role resulting in minor effects on gene regulation, or redundant gene regulation by other TFs. Collectively, these findings suggest that loss-of-function for single uncharacterized TFs might have limited phenotypic impacts but can reveal subsets of GRN predicted targets with altered expression.

玉米转录因子突变体的转录组图谱分析,探索基因调控网络预测。
转录因子(TFs)在调控基因表达和表型方面发挥着重要作用。目前已利用多种方法来开发基因调控网络(GRN),以预测每种 TF 的调控靶标,如酵母一杂交(Y1H)筛选和基因共表达网络(GCN)分析。在此,我们确定了潜在的 TF 靶标,并使用反向遗传学方法测试了玉米中几个 GRN 的预测结果。我们分离出了 22 个玉米 TF 的功能缺失突变等位基因。这些突变体没有表现出明显的形态表型。然而,转录组分析在每个突变基因型中都发现了不同的表达基因,靶向代谢分析表明一些突变体中存在不同的酚类积累。对基于 Y1H 筛选的预测靶基因的表达水平进行分析后发现,一小部分预测靶基因的表达水平发生了改变。对基于 GCN 方法的预测靶标的分析发现,一些 TF 的预测集有显著的富集,但大多数预测靶标并没有表现出表达的改变。这可能是由于 GCN 预测为假阳性、TF 的次级调控作用对基因调控的影响较小、或其他 TF 对基因的调控多余等原因造成的。总之,这些研究结果表明,单个未表征 TF 的功能缺失可能对表型的影响有限,但可以揭示出表达改变的 GRN 预测靶标子集。
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来源期刊
G3: Genes|Genomes|Genetics
G3: Genes|Genomes|Genetics GENETICS & HEREDITY-
CiteScore
5.10
自引率
3.80%
发文量
305
审稿时长
3-8 weeks
期刊介绍: G3: Genes, Genomes, Genetics provides a forum for the publication of high‐quality foundational research, particularly research that generates useful genetic and genomic information such as genome maps, single gene studies, genome‐wide association and QTL studies, as well as genome reports, mutant screens, and advances in methods and technology. The Editorial Board of G3 believes that rapid dissemination of these data is the necessary foundation for analysis that leads to mechanistic insights. G3, published by the Genetics Society of America, meets the critical and growing need of the genetics community for rapid review and publication of important results in all areas of genetics. G3 offers the opportunity to publish the puzzling finding or to present unpublished results that may not have been submitted for review and publication due to a perceived lack of a potential high-impact finding. G3 has earned the DOAJ Seal, which is a mark of certification for open access journals, awarded by DOAJ to journals that achieve a high level of openness, adhere to Best Practice and high publishing standards.
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