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循环致死毒素降低中性粒细胞对炭疽杆菌的反应能力。

Circulating lethal toxin decreases the ability of neutrophils to respond to Bacillus anthracis.

机构信息

Department of Microbiology, Immunology, and Cancer Biology, University of Virginia, Charlottesville, VA, USA.

出版信息

Cell Microbiol. 2014 Apr;16(4):504-18. doi: 10.1111/cmi.12232. Epub 2013 Nov 6.

Abstract

Polymorphonuclear leucocytes (PMNs) play a protective role during Bacillus anthracis infection. However, B. anthracis is able to subvert the PMN response effectively as evidenced by the high mortality rates of anthrax. One major virulence factor produced by B. anthracis, lethal toxin (LT), is necessary for dissemination in the BSL2 model of mouse infection. While human and mouse PMNs kill vegetative B. anthracis, short in vitro half-lives of PMNs have made it difficult to determine how or if LT alters their bactericidal function. Additionally, the role of LT intoxication on PMN's ability to migrate to inflammatory signals remains controversial. LF concentrations in both serum and major organs were determined from mice infected with B. anthracis Sterne strain at defined stages of infection to guide subsequent administration of purified toxin. Bactericidal activity of PMNs assessed using ex vivo cell culture assays showed significant defects in killing B. anthracis. In vivo PMN recruitment to inflammatory stimuli was significantly impaired at 24 h as assessed by real-time analysis of light-producing PMNs within the mouse. The observations described above suggest that LT serves dual functions; it both attenuates accumulation of PMNs at sites of inflammation and impairs PMNs bactericidal activity against vegetative B. anthracis.

摘要

多形核白细胞(PMN)在炭疽杆菌感染中发挥保护作用。然而,炭疽杆菌能够有效地颠覆 PMN 的反应,这从炭疽的高死亡率中可以明显看出。炭疽杆菌产生的一种主要毒力因子,致死毒素(LT),是在 BSL2 感染小鼠模型中传播所必需的。虽然人和鼠 PMN 可以杀死营养体炭疽杆菌,但 PMN 的体外半衰期较短,这使得很难确定 LT 是如何或是否改变了它们的杀菌功能。此外,LT 中毒对 PMN 向炎症信号迁移的能力的影响仍存在争议。从感染炭疽杆菌Sterne 株的小鼠的血清和主要器官中确定 LF 浓度,以指导随后纯化毒素的给药。使用体外细胞培养测定法评估 PMN 的杀菌活性,显示出对炭疽杆菌杀伤的明显缺陷。通过实时分析小鼠内产光 PMN ,在 24 小时时,PMN 向炎症刺激物的募集明显受损。上述观察结果表明,LT 具有双重功能;它既能减轻 PMN 在炎症部位的积聚,又能削弱 PMN 对营养体炭疽杆菌的杀菌活性。

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