Department of Microbiology, Miami University, Oxford, Ohio, USA.
Infect Immun. 2012 Mar;80(3):1015-24. doi: 10.1128/IAI.06279-11. Epub 2012 Jan 9.
Acinetobacter baumannii, which causes serious infections in immunocompromised patients, expresses high-affinity iron acquisition functions needed for growth under iron-limiting laboratory conditions. In this study, we determined that the initial interaction of the ATCC 19606(T) type strain with A549 human alveolar epithelial cells is independent of the production of BasD and BauA, proteins needed for acinetobactin biosynthesis and transport, respectively. In contrast, these proteins are required for this strain to persist within epithelial cells and cause their apoptotic death. Infection assays using Galleria mellonella larvae showed that impairment of acinetobactin biosynthesis and transport functions significantly reduces the ability of ATCC 19606(T) cells to persist and kill this host, a defect that was corrected by adding inorganic iron to the inocula. The results obtained with these ex vivo and in vivo approaches were validated using a mouse sepsis model, which showed that expression of the acinetobactin-mediated iron acquisition system is critical for ATCC 19606(T) to establish an infection and kill this vertebrate host. These observations demonstrate that the virulence of the ATCC 19606(T) strain depends on the expression of a fully active acinetobactin-mediated system. Interestingly, the three models also showed that impairment of BasD production results in an intermediate virulence phenotype compared to those of the parental strain and the BauA mutant. This observation suggests that acinetobactin intermediates or precursors play a virulence role, although their contribution to iron acquisition is less relevant than that of mature acinetobactin.
鲍曼不动杆菌会导致免疫功能低下的患者发生严重感染,它可以表达高亲和力的铁获取功能,以在缺铁的实验室条件下生长。在这项研究中,我们确定 ATCC 19606(T) 型菌株与 A549 人肺泡上皮细胞的初始相互作用不依赖于 BasD 和 BauA 的产生,这两种蛋白分别是用于 Acinetobactin 生物合成和运输所必需的。相比之下,这些蛋白对于该菌株在上皮细胞内持续存在并导致其凋亡死亡是必需的。使用金龟子幼虫进行的感染实验表明,Acinetobactin 生物合成和运输功能的损伤显著降低了 ATCC 19606(T) 细胞在这种宿主中持续存在和杀死的能力,而向接种物中添加无机铁可以纠正这种缺陷。使用小鼠脓毒症模型验证了这些离体和体内方法的结果,表明 Acinetobactin 介导的铁获取系统的表达对于 ATCC 19606(T) 建立感染并杀死这种脊椎动物宿主至关重要。这些观察结果表明,ATCC 19606(T) 菌株的毒力取决于完全活性的 Acinetobactin 介导系统的表达。有趣的是,这三个模型还表明,与亲本菌株和 BauA 突变体相比,BasD 产生的损伤导致中间毒力表型。这一观察结果表明,Acinetobactin 中间体或前体发挥毒力作用,尽管它们对铁获取的贡献不如成熟 Acinetobactin 重要。