转录因子
结核分枝杆菌
基因调控网络
缺氧(环境)
生物
分解代谢
合成代谢
基因表达
计算生物学
基因表达谱
基因
细胞生物学
肺结核
抄写(语言学)
基因表达调控
遗传学
化学
氧气
生物化学
新陈代谢
医学
病理
哲学
有机化学
语言学
作者
James E. Galagan,K Minch,Matthew Peterson,Anna Lyubetskaya,Elham Azizi,Linsday Sweet,Antonio L. C. Gomes,Tige R. Rustad,Gregory Dolganov,Irina Glotova,Thomas Abeel,Chris Mahwinney,Adam D. Kennedy,René Allard,William Brabant,Andrew Krueger,Suma Jaini,Brent Honda,Wen‐Han Yu,Mark J. Hickey
出处
期刊:Nature
[Springer Nature]
日期:2013-07-01
卷期号:499 (7457): 178-183
被引量:440
摘要
We have taken the first steps towards a complete reconstruction of the Mycobacterium tuberculosis regulatory network based on ChIP-Seq and combined this reconstruction with system-wide profiling of messenger RNAs, proteins, metabolites and lipids during hypoxia and re-aeration. Adaptations to hypoxia are thought to have a prominent role in M. tuberculosis pathogenesis. Using ChIP-Seq combined with expression data from the induction of the same factors, we have reconstructed a draft regulatory network based on 50 transcription factors. This network model revealed a direct interconnection between the hypoxic response, lipid catabolism, lipid anabolism and the production of cell wall lipids. As a validation of this model, in response to oxygen availability we observe substantial alterations in lipid content and changes in gene expression and metabolites in corresponding metabolic pathways. The regulatory network reveals transcription factors underlying these changes, allows us to computationally predict expression changes, and indicates that Rv0081 is a regulatory hub.
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