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本文引用的文献

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A new mycobacterial infection in man.人类的一种新的分枝杆菌感染。
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A novel mycolactone from a clinical isolate of Mycobacterium ulcerans provides evidence for additional toxin heterogeneity as a result of specific changes in the modular polyketide synthase.从溃疡分枝杆菌临床分离株中获得的一种新型分枝杆菌内酯,为模块化聚酮合酶的特定变化导致毒素异质性增加提供了证据。
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Common evolutionary origin for the unstable virulence plasmid pMUM found in geographically diverse strains of Mycobacterium ulcerans.在地理分布多样的溃疡分枝杆菌菌株中发现的不稳定毒力质粒pMUM的共同进化起源。
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Cytokine responses to stimulation of whole blood from patients with Buruli ulcer disease in Ghana.加纳布氏菌病患者全血刺激后的细胞因子反应。
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Mycobacterium ulcerans disease: role of age and gender in incidence and morbidity.溃疡分枝杆菌病:年龄和性别在发病率及发病情况中的作用
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A mycobacterial virulence gene cluster extending RD1 is required for cytolysis, bacterial spreading and ESAT-6 secretion.一个延伸RD1的分枝杆菌毒力基因簇对于细胞溶解、细菌扩散和ESAT-6分泌是必需的。
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Buruli ulcer disease in Cameroon rediscovered.喀麦隆再次发现布氏杆菌溃疡病。
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Immunity to tuberculosis.对结核病的免疫力。
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Differential production of systemic and intralesional gamma interferon and interleukin-10 in nodular and ulcerative forms of Buruli disease.布氏杆菌病结节型和溃疡型中全身及病灶内γ干扰素和白细胞介素-10的差异产生
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溃疡分枝杆菌感染会在小鼠体内引发持续的炎症反应。

Infection with Mycobacterium ulcerans induces persistent inflammatory responses in mice.

作者信息

Oliveira Martinha S, Fraga Alexandra G, Torrado Egídio, Castro António G, Pereira João P, Filho Adhemar Longatto, Milanezi Fernanda, Schmitt Fernando C, Meyers Wayne M, Portaels Françoise, Silva Manuel T, Pedrosa Jorge

机构信息

Life and Health Sciences Research Institute, School of Health Sciences (ICVS), University of Minho, Braga, Portugal.

出版信息

Infect Immun. 2005 Oct;73(10):6299-310. doi: 10.1128/IAI.73.10.6299-6310.2005.

DOI:10.1128/IAI.73.10.6299-6310.2005
PMID:16177301
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1230890/
Abstract

Buruli ulcer (BU) is a devastating, necrotizing, tropical skin disease caused by infections with Mycobacterium ulcerans. In contrast to other mycobacterioses, BU has been associated with minimal or absent inflammation. However, here we show that in the mouse M. ulcerans induces persistent inflammatory responses with virulence-dependent patterns. Mycolactone-positive, cytotoxic strains are virulent for mice and multiply progressively, inducing both early and persistent acute inflammatory responses. The cytotoxicity of these strains leads to progressive destruction of the inflammatory infiltrates by postapoptotic secondary necrosis, generating necrotic acellular areas with extracellular bacilli released by the lysis of infected phagocytes. The necrotic areas, always surrounded by acute inflammatory infiltrates, expand through the progressive invasion of healthy tissues around the initial necrotic lesions by bacteria and by newly recruited acute inflammatory cells. Our observations show that the lack of inflammatory infiltrates in the extensive areas of necrosis seen in advanced infections results from the destruction of continuously produced inflammatory infiltrates and not from M. ulcerans-induced local or systemic immunosuppression. Whether this is the mechanism behind the predominance of minimal or absent inflammatory responses in BU biopsies remains to be elucidated.

摘要

布鲁里溃疡(BU)是一种由溃疡分枝杆菌感染引起的毁灭性坏死性热带皮肤病。与其他分枝杆菌病不同,布鲁里溃疡与轻微炎症或无炎症相关。然而,我们在此表明,在小鼠中,溃疡分枝杆菌会引发具有毒力依赖性模式的持续性炎症反应。产生嗜肉毒素的细胞毒性菌株对小鼠具有致病性,并会逐渐增殖,引发早期和持续性急性炎症反应。这些菌株的细胞毒性会导致炎症浸润细胞发生凋亡后继发性坏死,进而导致炎症浸润逐渐破坏,产生坏死无细胞区域,其中含有因被感染吞噬细胞裂解而释放的细胞外杆菌。坏死区域总是被急性炎症浸润所包围,并通过细菌和新招募的急性炎症细胞对初始坏死病变周围健康组织的逐步侵袭而扩大。我们的观察结果表明,在晚期感染中广泛坏死区域缺乏炎症浸润是由于持续产生的炎症浸润被破坏,而非溃疡分枝杆菌诱导的局部或全身免疫抑制所致。这是否是布鲁里溃疡活检中炎症反应轻微或无炎症反应占主导的机制仍有待阐明。