Polymorphic potential of SRF binding site of c-Fos gene promoter: in vitro study†

IF 4.6 3区 化学 Q2 CHEMISTRY, MULTIDISCIPLINARY RSC Advances Pub Date : 2024-12-03 DOI:10.1039/D4RA05897F
Barbora Profantová, Václav Římal, Václav Profant, Ondřej Socha, Ivan Barvík, Helena Štěpánková and Josef Štěpánek
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Abstract

Recently published in vivo observations have highlighted the presence of cruciform structures within the genome, suggesting their potential significance in the rapid recognition of the target sequence for transcription factor binding. In this in vitro study, we investigate the organization and stability of the sense (coding) strand within the Serum Response Element of the c-Fos gene promoter (c-Fos SRE), specifically focusing on segments spanning 12 to 36 nucleotides, centered around the CArG-box. Through a thorough examination of UV absorption patterns with varying temperatures, we identified the emergence of a remarkably stable structure, which we conclusively characterized as a hairpin using complementary 1H NMR experiments. Our research decisively ruled out the formation of homoduplexes, as confirmed by supplementary fluorescence experiments. Utilizing molecular dynamics simulations with atomic distance constraints derived from NMR data, we explored the structural intricacies of the compact hairpin. Notably, the loop consisting of the six-membered A/T sequence demonstrated substantial stabilization through extensive stacking, non-canonical inter-base hydrogen bonding, and hydrophobic clustering of thymine methyl groups. These findings suggest the potential of the c-Fos SRE to adopt a cruciform structure (consisting of two opposing hairpins), potentially providing a topological recognition site for the SRF transcription factor under cellular conditions. Our results should inspire further biochemical and in vivo studies to explore the functional implications of these non-canonical DNA structures.

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c-Fos基因启动子SRF结合位点的多态性潜力:体外研究
最近发表的体内观察强调了基因组中十字形结构的存在,表明它们在转录因子结合靶序列的快速识别中具有潜在的重要意义。在这项体外研究中,我们研究了c-Fos基因启动子(c-Fos SRE)血清反应元件中意义(编码)链的组织和稳定性,特别关注了以CArG-box为中心的12至36个核苷酸的片段。通过对不同温度下紫外线吸收模式的彻底检查,我们发现了一个非常稳定的结构的出现,我们最终用互补的1H NMR实验将其定性为发夹。我们的研究果断地排除了同型双工的形成,补充荧光实验证实了这一点。利用基于核磁共振数据的原子距离约束的分子动力学模拟,我们探索了紧凑发夹的结构复杂性。值得注意的是,由六元A/T序列组成的环通过广泛的堆叠、非规范的碱基间氢键和胸腺嘧啶甲基的疏水聚类显示出实质性的稳定性。这些发现表明c-Fos SRE可能采用十字形结构(由两个相反的发夹组成),可能在细胞条件下为SRF转录因子提供拓扑识别位点。我们的结果应该启发进一步的生化和体内研究,以探索这些非规范DNA结构的功能意义。
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来源期刊
RSC Advances
RSC Advances chemical sciences-
CiteScore
7.50
自引率
2.60%
发文量
3116
审稿时长
1.6 months
期刊介绍: An international, peer-reviewed journal covering all of the chemical sciences, including multidisciplinary and emerging areas. RSC Advances is a gold open access journal allowing researchers free access to research articles, and offering an affordable open access publishing option for authors around the world.
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