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铁摄取调节蛋白及其在非典型流感嗜血杆菌发病机制中的作用。

Ferric uptake regulator and its role in the pathogenesis of nontypeable Haemophilus influenzae.

机构信息

The Center for Microbial Pathogenesis, The Research Institute at Nationwide Children's Hospital, The Center for Microbial Interface Biology, and Department of Pediatrics, The Ohio State University, Columbus, Ohio, USA.

出版信息

Infect Immun. 2013 Apr;81(4):1221-33. doi: 10.1128/IAI.01227-12. Epub 2013 Feb 4.

Abstract

Nontypeable Haemophilus influenzae (NTHi) is a commensal microorganism of the human nasopharynx, and yet is also an opportunistic pathogen of the upper and lower respiratory tracts. Host microenvironments influence gene expression patterns, likely critical for NTHi persistence. The host sequesters iron as a mechanism to control microbial growth, and yet iron limitation influences gene expression and subsequent production of proteins involved in iron homeostasis. Careful regulation of iron uptake, via the ferric uptake regulator Fur, is essential in multiple bacteria, including NTHi. We hypothesized therefore that Fur contributes to iron homeostasis in NTHi, is critical for bacterial persistence, and likely regulates expression of virulence factors. Toward this end, fur was deleted in the prototypic NTHi clinical isolate, 86-028NP, and we assessed gene expression regulated by Fur. As expected, expression of the majority of genes that encode proteins with predicted roles in iron utilization was repressed by Fur. However, 14 Fur-regulated genes encode proteins with no known function, and yet may contribute to iron utilization or other biological functions. In a mammalian model of human otitis media, we determined that Fur was critical for bacterial persistence, indicating an important role for Fur-mediated iron homeostasis in disease progression. These data provide a profile of genes regulated by Fur in NTHi and likely identify additional regulatory pathways involved in iron utilization. Identification of such pathways will increase our understanding of how this pathogen can persist within host microenvironments, as a common commensal and, importantly, as a pathogen with significant clinical impact.

摘要

无乳链球菌(NTHi)是人类鼻咽部的共生微生物,但也是上呼吸道和下呼吸道的机会性病原体。宿主微环境影响基因表达模式,这可能对 NTHi 的持续存在至关重要。宿主将铁隔离作为控制微生物生长的一种机制,但铁限制会影响基因表达和随后参与铁稳态的蛋白质的产生。通过铁摄取调节剂 Fur 对铁摄取进行精细调节,对包括 NTHi 在内的多种细菌都是必不可少的。因此,我们假设 Fur 有助于 NTHi 中的铁稳态,对细菌的持续存在至关重要,并且可能调节毒力因子的表达。为此,我们在原型 NTHi 临床分离株 86-028NP 中缺失了 fur,并评估了 Fur 调节的基因表达。正如预期的那样,编码预测在铁利用中具有作用的蛋白质的大多数基因的表达受到 Fur 的抑制。然而,14 个 Fur 调节基因编码具有未知功能的蛋白质,但可能有助于铁利用或其他生物学功能。在人类中耳炎的哺乳动物模型中,我们确定 Fur 对于细菌的持续存在至关重要,表明 Fur 介导的铁稳态在疾病进展中起着重要作用。这些数据提供了 NTHi 中 Fur 调节基因的图谱,并可能确定了参与铁利用的其他调节途径。识别这些途径将增加我们对这种病原体如何在宿主微环境中持续存在的理解,作为一种常见的共生体,以及重要的是,作为一种具有重大临床影响的病原体。

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