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Comprehensive analysis of iron utilization by Mycobacterium tuberculosis

机译:结核分枝杆菌铁利用综合分析

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Iron is essential for nearly all bacterial pathogens, including Mycobacterium tuberculosis (Mtb), but is severely limited in the human host. To meet its iron needs, Mtb secretes siderophores, small molecules with high affinity for iron, and takes up iron-loaded mycobactins (MBT) and carboxymycobactins (cMBT), from the environment. Mtb is also capable of utilizing heme and hemoglobin which contain more than 70% of the iron in the human body. However, many components of these iron acquisition pathways are still unknown. In this study, a high-density transposon mutagenesis coupled with deep sequencing (TnSeq) showed that Mtb exhibits nearly opposite requirements for 165 genes in the presence of heme and hemoglobin versus MBT and cMBT as iron sources. The ESX-3 secretion system was assessed as essential for siderophore-mediated iron uptake and, surprisingly, also for heme utilization by Mtb. Predictions derived from the TnSeq analysis were validated by growth experiments with isogenic Mtb mutants. These results showed that (i) the efflux pump MmpL5 plays a dominant role in siderophore secretion, (ii) the Rv2047c protein is essential for growth of Mtb in the presence of mycobactin, and (iii) the transcriptional repressor Zur is required for heme utilization by Mtb. The novel genetic determinants of iron utilization revealed in this study will stimulate further experiments in this important area of Mtb physiology.
机译:铁对几乎所有细菌病原体都必须,包括结核分枝杆菌(MTB),但在人宿主中受到严重限制。为了满足其铁需求,MTB分泌施工团,具有高亲和力的小分子,从环境中占用铁载霉菌素(MBT)和羧基酰甲酰胺(CMBT)。 MTB还能够利用血红素和血红蛋白,其含有超过70%的人体中的铁。然而,这些铁采集途径的许多组件仍然未知。在该研究中,与深序列(TNSeq)偶联的高密度转座子诱变表明,MTB在血红素和血红蛋白存在与MBT和CMBT作为铁源的情况下表现出对165个基因的几乎相反的要求。 ESX-3分泌系统被评估为纵向介导的铁摄取至关重要,并且令人惊讶的是MTB的血红素利用。通过具有同种型MTB突变体的生长实验,验证了从TNSeq分析衍生的预测。这些结果表明,(i)流出泵MMPL5在西参分泌中起主要作用,(ii)RV2047C蛋白在霉菌蛋白存在下MTB的生长至关重要,(iii)血红素利用所需的转录阻遏物Zur是必不可少的通过MTB。本研究中揭示的铁利用的新遗传决定因素将刺激MTB生理学的这一重要领域进一步的实验。

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