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5-氮杂胞苷对嗜水角根霉的表观遗传调控增强了抗真菌代谢产物的产生:来自抗菌、代谢、基因组和计算分析的见解

Epigenetic modulation of Ceratorhiza hydrophila by 5-azacytidine enhances antifungal metabolite production: insights from antimicrobial, metabolic, genomic and computational analyses.

作者信息

Abdelhamid Rehab M, Soliman Elham R S, Mohamed Eslam T, Elsaba Yasmin M

机构信息

Botany and Microbiology Department, Faculty of Science, Helwan University, Cairo, 11421, Egypt.

出版信息

BMC Microbiol. 2025 Sep 9;25(1):574. doi: 10.1186/s12866-025-04330-8.

Abstract

BACKGROUND

The emergence of drug-resistant pathogens has stimulated the need for the development of new antimicrobial agents. Epigenetic modulation by suppressing epigenetic inhibitors, such as 5-azacytidine (5-aza), has been shown to activate silent biosynthetic gene clusters within a fungus and causes the production of novel secondary metabolites. This research examined this epigenetic modification strategy in the poorly studied filamentous fungus, Ceratorhiza hydrophila, which may help induce the additional production of bioactive compounds.

RESULTS

The results from genomic and spectroscopic analyses (ISSR profiling and FTIR spectroscopy) indicated that 50 µM 5-aza produced substantial global DNA demethylation and genomic changes in C. hydrophila with no impact on cell viability. The epigenetic changes associated with the DNA demethylation prompted a notable and selective change in antimicrobial profile to suppress antibacterial activity against strains such as Clostridium sporogenes while also showing a robust induction of antifungal activity against Candida albicans (22 mm inhibition zone). GC-MS was performed for a deep-dive characterization of the metabolic profile which revealed, for example, a dramatic alteration of the profile including production of new secondary metabolites such as a novel indole derivative and diisooctyl phthalate, which did not exist in the untreated control. In silico analyses, such as modelling the promoter and molecular docking opportunities, offered a believable mechanistic rationale for the effects seen, linked to the predicted modulation of primary biosynthetic pathways.

CONCLUSION

This study demonstrates that epigenetic modulation can be used to successfully unlock latent biosynthetic capability in C. hydrophila resulting in the production of unique compounds with strong and selective antifungal activity. These results demonstrate the advantages of epigenetic screening of unique fungal sources in the search for new drug leads.

摘要

背景

耐药病原体的出现激发了开发新型抗菌剂的需求。通过抑制表观遗传抑制剂(如5-氮杂胞苷(5-aza))进行表观遗传调控,已被证明可激活真菌内沉默的生物合成基因簇,并导致产生新的次生代谢产物。本研究在研究较少的丝状真菌嗜水角喙霉中考察了这种表观遗传修饰策略,这可能有助于诱导生物活性化合物的额外产生。

结果

基因组和光谱分析(ISSR谱分析和傅里叶变换红外光谱)结果表明,50μM的5-aza在嗜水角喙霉中产生了大量的全基因组DNA去甲基化和基因组变化,且对细胞活力无影响。与DNA去甲基化相关的表观遗传变化促使抗菌谱发生显著且选择性的变化,抑制了对诸如产芽孢梭菌等菌株的抗菌活性,同时也显示出对白色念珠菌的强大抗真菌活性诱导作用(抑菌圈为22毫米)。进行了气相色谱-质谱联用分析以深入表征代谢谱,结果揭示了例如谱图的显著改变,包括产生了新的次生代谢产物,如一种新型吲哚衍生物和邻苯二甲酸二异辛酯,而这些在未处理的对照中并不存在。诸如对启动子进行建模和分子对接机会等计算机模拟分析,为所观察到的效应提供了可信的作用机制原理,这与初级生物合成途径的预测调控相关。

结论

本研究表明,表观遗传调控可成功解锁嗜水角喙霉中潜在的生物合成能力,从而产生具有强大且选择性抗真菌活性的独特化合物。这些结果证明了在寻找新的药物先导物时对独特真菌来源进行表观遗传筛选的优势。

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