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Identification and characterization of an Acinetobacter baumannii biofilm-associated protein.

机译:鲍曼不动杆菌生物膜相关蛋白的鉴定和表征。

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摘要

Acinetobacter baumannii is a Gram-negative bacterium that has emerged recently as an important nosocomial opportunistic pathogen. In 1975, Acinetobacter species accounted for 1.5 and 1.8% of bacterial isolates associated with nosocomial pneumonia and bloodstream infection, respectively, and by 2003, had increased to 6.9 and 2.4% (39). There are an estimated 1.7 million healthcare-associated infections each year in the US, and 67,000 deaths due to hospital-acquired pneumonia and bloodstream infection (61), so Acinetobacter infection is estimated to cause 3200 deaths each year, in addition to significant morbidity costs. With an unusual ability to persist on dry surfaces for months (54, 64) and remarkable intrinsic and acquired resistance to antibiotics (11, 136), Acinetobacter is likely to remain a problem for hospitals and patients worldwide.;We have identified a large biofilm-associated protein (Bap) present on the surface of a bloodstream isolate of A. baumannii.We have developed anti-Bap monoclonal antibody (MAb) 6E3, which reacts with 43% of the isolates in our library of clinically-relevant Acinetobacter species, and anti-Bap polyclonal antibody, which reacts with 33% of the isolates. We have analyzed each of the isolates in a semi-quantitative biofilm assay, and demonstrated that for A. baumannii strain 307-0294, Bap is required for wild-type biofilm formation.;We have determined that bap transcript abundance is increased during late logarithmic and stationary phases of the bacterial growth curve, likely in response to a diffusible signaling molecule released into the media. Once induced, bap transcript levels are maintained by a cell-density-dependent mechanism, possibly in response to physical cell-cell contact signaling. Consistent with these results, confocal immunofluorescent microscopy of mature biofilms stained with MAb 6E3 demonstrate that Bap is expressed by stationary cells within microcolonies adherent to a glass coverslip, but not by planktonic cells coursing through water channels within and floating above the biofilm structure. Finally, we have identified an outer-membrane protein that co-immunoprecipitates with Bap and is absent from outer-membrane preparations of the Bap-deficient mutant bap1302::EZ-Tn5, suggesting that these two proteins interact on the surface of A. baumannii.;Acinetobacter colonization of the hospital environment presents a serious threat to vulnerable patients requiring invasive medical devices. Biofilm formation may contribute to the ability of Acinetobacter to persist in the hospital environment, and a thorough understanding of factors that contribute to biofilm formation may facilitate effective disinfection and treatment.
机译:鲍曼不动杆菌是革兰氏阴性细菌,最近作为重要的医院机会病原体出现。 1975年,不动杆菌属分别占与医院内肺炎和血流感染有关的细菌分离株的1.5%和1.8%,到2003年,增加到6.9%和2.4%(39)。在美国,每年估计有170万与医疗相关的感染,以及因医院获得性肺炎和血流感染而导致的67,000例死亡(61),因此,除重大的发病费用外,不动杆菌的感染估计每年导致3200例死亡。 。由于不寻常的能力可以在干燥的表面上持续数月(54,64),并且对抗生素具有显着的内在和后天抵抗力(11,136),不动杆菌可能仍然是全球医院和患者的问题。鲍曼不动杆菌血流分离物表面上存在相关蛋白(Bap)。我们开发了抗Bap单克隆抗体(MAb)6E3,可与我们临床相关不动杆菌属文库中的43%分离物反应,抗Bap多克隆抗体,可与33%的分离物反应。我们通过半定量生物膜分析法对每种分离物进行了分析,并证明对于鲍曼不动杆菌菌株307-0294,Bap是野生型生物膜形成所必需的;我们已确定在对数后期,bap转录本的丰度增加了。细菌生长曲线的固定阶段和固定阶段,可能是由于释放到培养基中的可扩散信号分子引起的。一旦被诱导,bap转录物水平通过细胞密度依赖性机制维持,可能响应于物理细胞-细胞接触信号传导。与这些结果一致,用MAb 6E3染色的成熟生物膜的共聚焦免疫荧光显微镜检查表明,Bap由粘附在玻璃盖玻片上的微菌落中的固定细胞表达,但不是通过游动通过生物膜结构内部和上方漂浮的水通道的浮游细胞表达的。最后,我们确定了一种与Bap共同免疫沉淀的外膜蛋白,而Bap缺陷型突变体bap1302 :: EZ-Tn5的外膜制剂中没有这种蛋白,表明这两种蛋白在鲍曼不动杆菌的表面相互作用。 。;不动杆菌在医院环境中的定殖对需要侵入式医疗设备的脆弱患者构成了严重威胁。生物膜的形成可能有助于不动杆菌在医院环境中持续存在的能力,并且对导致生物膜形成的因素的透彻了解可以促进有效的消毒和治疗。

著录项

  • 作者

    Loehfelm, Thomas William.;

  • 作者单位

    State University of New York at Buffalo.;

  • 授予单位 State University of New York at Buffalo.;
  • 学科 Biology Molecular.;Biology Microbiology.;Health Sciences General.
  • 学位 Ph.D.
  • 年度 2010
  • 页码 139 p.
  • 总页数 139
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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