与 QT 间期相关的 SCN5A 增强子变异的功能表征确定了综合叠加效应。

IF 3.3 Q2 GENETICS & HEREDITY HGG Advances Pub Date : 2024-09-30 DOI:10.1016/j.xhgg.2024.100358
Lavanya Gunamalai, Parul Singh, Brian Berg, Leilei Shi, Ernesto Sanchez, Alexa Smith, Ghislain Breton, Mark T Bedford, Darius Balciunas, Ashish Kapoor
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引用次数: 0

摘要

一些经验和理论研究表明,每个基因存在多个增强子,共同调控基因表达,而影响这些增强子活动的共同序列变异是个体间基因表达变异的主要来源。然而,对于绝大多数基因来说,增强子及其背后的调控变异仍然是未知的。即使是那些增强子特征明确的基因,多个增强子及其变体(如果已知)对基因表达调控的联合效应的性质也仍未得到探索。在这里,我们评估了五个 SCN5A 增强子及其调控变体的联合效应,已知这些增强子及其调控变体与 SCN5A 的心脏表达共同相关,并且是一般人群中 QT 间期关联的基础。在小鼠心肌细胞系的外显子报告实验中,我们利用以调控变体为中心的小缺失,证明这些变体及其侧翼序列在单个增强子的活动中起着关键作用,很可能是转录因子(TF)的结合位点。通过对预测的转录因子进行寡核苷酸下拉检测,我们确定了可能驱动等位基因特异性增强子活动的转录因子。在报告实验中使用所有 32 个可能的等位基因合成构建物(代表五个双等位基因增强子),我们证明了对整体增强子活动的综合加成效应。利用斑马鱼胚胎中的瞬时增强子实验,我们证明有四个元件在体内起着增强子的作用。这些研究共同揭示了驱动 QT 间期相关 SCN5A 调控变体增强子活性的 TFs,揭示了这些调控变体等位基因组合的叠加效应,并证明了它们在体内作为增强子的潜力。
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Functional characterization of QT interval associated SCN5A enhancer variants identify combined additive effects.

Several empirical and theoretical studies suggest the presence of multiple enhancers per gene that collectively regulate gene expression, and that common sequence variation impacting on the activities of these enhancers is a major source of inter-individual gene expression variability. However, for the vast majority of genes, enhancers and the underlying regulatory variation remains unknown. Even for the genes with well-characterized enhancers, the nature of the combined effects from multiple enhancers and their variants, when known, on gene expression regulation remains unexplored. Here, we have evaluated the combined effects from five SCN5A enhancers and their regulatory variants that are known to collectively correlate with SCN5A cardiac expression and underlie QT interval association in the general population. Using small deletions centered at the regulatory variants in episomal reporter assays in a mouse cardiomyocyte cell line, we demonstrate that the variants and their flanking sequences play critical role in individual enhancer activities, likely being a transcription factor (TF) binding site. By oligonucleotide-based pulldown assays on predicted TFs, we identify the TFs likely driving allele-specific enhancer activities. Using all 32 possible allelic synthetic constructs in reporter assays, representing the five bi-allelic enhancers, we demonstrate combined additive effects on overall enhancer activities. Using transient enhancer assays in zebrafish embryos we demonstrate that four elements act as enhancers in vivo. Together, these studies uncover the TFs driving the enhancer activities of QT interval associated SCN5A regulatory variants, reveal the additive effects from allelic combinations of these regulatory variants, and prove their potential to act as enhancers in vivo.

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来源期刊
HGG Advances
HGG Advances Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
4.30
自引率
4.50%
发文量
69
审稿时长
14 weeks
期刊最新文献
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