Transcriptional profiling of Mycobacterium smegmatis exposed to subinhibitory concentrations of G4-stabilizing ligands

IF 0.2 Q4 MEDICINE, GENERAL & INTERNAL
MV Zaychikova, D. Bespiatykh, M. Malakhova, IN Bodoev, TS Vedekhina, V. Veselovsky, KM Klimina, AM Varizhuk, E. Shitikov
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引用次数: 0

Abstract

The spread of Mycobacterium tuberculosis drug resistance accentuates the demand for anti-tuberculosis drugs with a fundamentally new mechanism of action without conferring cross-resistance. G-quadruplexes (G4, non-canonical DNA structures) are plausible new drug targets. Although G4-stabilizing ligands have been shown to inhibit mycobacterial growth, the exact mechanism of their action is uncertain. The aim of this study was to assess a possible correlation between putative G4 elements in a model mycobacterial strain M. smegmatis MC2155 and transcriptomic changes under the action of subinhibitory concentrations of G4 ligands BRACO-19 and TMPyP4. We also planned to compare the results with corresponding data previously obtained by us using higher, inhibitory concentrations of these ligands. For BRACO-19, we identified 589 (316↑; 273↓) and 865 (555↑; 310↓) differentially expressed genes at 5 µМ and 10 µМ, respectively. For TMPyP4, we observed the opposite trend, the number of differentially expressed genes decreased at higher concentration of the ligand: 754 (337↑; 417↓) and 702 (359↑; 343↓) for 2 µМ and 4 µМ, respectively. Statistical analysis revealed no correlation between ligand-induced transcriptomic changes and genomic localization of the putative quadruplex-forming sequences. At the same time, the data indicate certain functional specificity of the ligand-mediated transcriptomic effects, with TMPyP4 significantly affecting expression levels of transcription factors and arginine biosynthesis genes and BRACO-19 significantly affecting expression levels of iron metabolism and replication and reparation system genes.
暴露于低抑制浓度G4稳定配体的耻垢分枝杆菌的转录谱
结核分枝杆菌耐药性的传播加剧了对抗结核药物的需求,这种药物具有一种全新的作用机制,不会产生交叉耐药性。G-四链体(G4,非经典DNA结构)是可能的新药靶点。尽管G4稳定配体已被证明能抑制分枝杆菌的生长,但其确切作用机制尚不确定。本研究的目的是评估模型分枝杆菌菌株耻垢分枝杆菌MC2155中推定的G4元素与G4配体BRACO-19和TMPyP4亚抑制浓度作用下的转录组变化之间的可能相关性。我们还计划将结果与之前使用这些配体的更高抑制浓度获得的相应数据进行比较。对于BRACO-19,我们确定589(316↑; 273↓) 和865(555↑; 310↓) 分别在5µМ和10µМ处差异表达的基因。对于TMPyP4,我们观察到相反的趋势,在更高浓度的配体下,差异表达基因的数量减少:754(337↑; 417↓) 和702(359↑; 343↓) 分别为2µМ和4µМ。统计分析显示配体诱导的转录组变化和假定的四链体形成序列的基因组定位之间没有相关性。同时,数据表明配体介导的转录组效应具有一定的功能特异性,TMPyP4显著影响转录因子和精氨酸生物合成基因的表达水平,BRACO-19显著影响铁代谢和复制修复系统基因的表达。
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来源期刊
Bulletin of Russian State Medical University
Bulletin of Russian State Medical University MEDICINE, GENERAL & INTERNAL-
CiteScore
0.80
自引率
0.00%
发文量
59
期刊介绍: Bulletin of Russian State Medical University (Bulletin of RSMU, ISSN Print 2500–1094, ISSN Online 2542–1204) is a peer-reviewed medical journal of Pirogov Russian National Research Medical University (Moscow, Russia). The original language of the journal is Russian (Vestnik Rossiyskogo Gosudarstvennogo Meditsinskogo Universiteta, Vestnik RGMU, ISSN Print 2070–7320, ISSN Online 2070–7339). Founded in 1994, it is issued once every two months publishing articles on clinical medicine and medical and biological sciences, first of all oncology, neurobiology, allergy and immunology, medical genetics, medical microbiology and infectious diseases. Every issue is thematic. Deadlines for manuscript submission are announced in advance. The number of publications on topics in spite of the issue topic is limited. The journal accepts only original articles submitted by their authors, including articles that present methods and techniques, clinical cases and opinions. Authors must guarantee that their work has not been previously published elsewhere in whole or in part and in other languages and is not under consideration by another scientific journal. The journal publishes only one review per issue; the review is ordered by the editors.
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