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羊种布鲁氏菌、沙漠林鼠布鲁氏菌和绵羊布鲁氏菌引发常见且独特的巨噬细胞防御转录反应。

Brucella melitensis, B. neotomae and B. ovis elicit common and distinctive macrophage defense transcriptional responses.

作者信息

Covert Jill, Mathison Angela J, Eskra Linda, Banai Menachem, Splitter Gary

机构信息

University of Wisconsin-Madison, 1656 Linden Dr., Madison, WI 53706, USA.

出版信息

Exp Biol Med (Maywood). 2009 Dec;234(12):1450-67. doi: 10.3181/0904-RM-124.

Abstract

Brucella spp. establish an intracellular replicative niche in macrophages, while macrophages attempt to eliminate the bacteria by innate defense mechanisms. Brucella spp. possess similar genomes yet exhibit different macrophage infections. Few B. melitensis and B. neotomae enter macrophages with intracellular adaptation occurring over 4-8 hr. Conversely, B. ovis are readily ingested by macrophages and exhibit a persistent plateau of infection. Evaluating early macrophage interaction with Brucella spp. allows discovery of host entry and intracellular translocation mechanisms. Microarray analysis of macrophage transcriptional response following a 4 hr infection by different Brucella spp. revealed common macrophage genes altered in expression compared to uninfected macrophages. Macrophage infection with three different Brucella spp. provokes a common innate immune theme with increased transcript levels of chemokines and defense response genes and decreased transcript levels of GTPase signaling and cytoskeletal function that may affect trafficking of Brucella containing vesicles. For example, transcript levels of genes associated with chemotaxis (IL-1beta, MIP-1alpha), cytokine regulation (Socs3) and defense (Fas, Tnf) were increased, while transcript levels of genes associated with vesicular trafficking (Rab3d) and lysosomal associated enzymes (prosaposin) were decreased. Genes with altered macrophage transcript levels among Brucella spp. infections may correlate with species specific host defenses and intracellular survival strategies. Depending on the infecting Brucella species, gene ontology categorization identified genes differentially involved in cell growth and maintenance, endopeptidase inhibitor activity and G-protein mediated signaling. Examples of decreased gene expression in B. melitensis infection but not other Brucella spp. were growth arrest (Gas2), immunoglobulin receptor (FcgammarI) and chemokine receptor (Cxcr4) genes, suggesting opposing effects on intracellular functions.

摘要

布鲁氏菌属在巨噬细胞内建立一个胞内复制龛,而巨噬细胞试图通过固有防御机制清除细菌。布鲁氏菌属拥有相似的基因组,但表现出不同的巨噬细胞感染情况。很少有羊种布鲁氏菌和新墨西哥州布鲁氏菌进入巨噬细胞,胞内适应过程发生在4至8小时。相反,绵羊布鲁氏菌很容易被巨噬细胞摄取,并呈现出持续稳定的感染状态。评估巨噬细胞与布鲁氏菌属的早期相互作用有助于发现宿主进入和胞内转运机制。对不同布鲁氏菌属感染4小时后巨噬细胞转录反应进行微阵列分析,结果显示与未感染的巨噬细胞相比,有一些共同的巨噬细胞基因表达发生了改变。用三种不同的布鲁氏菌属感染巨噬细胞引发了一个共同的固有免疫主题,趋化因子和防御反应基因的转录水平升高,而GTPase信号传导和细胞骨架功能的转录水平降低,这可能会影响含布鲁氏菌小泡的运输。例如,与趋化性(IL-1β、MIP-1α)、细胞因子调节(Socs3)和防御(Fas、Tnf)相关的基因转录水平升高,而与小泡运输(Rab3d)和溶酶体相关酶(prosaposin)相关的基因转录水平降低。在布鲁氏菌属感染中巨噬细胞转录水平发生改变的基因可能与物种特异性的宿主防御和胞内存活策略相关。根据感染的布鲁氏菌种类,基因本体分类鉴定出在细胞生长和维持、内肽酶抑制剂活性以及G蛋白介导的信号传导中差异参与的基因。在羊种布鲁氏菌感染中基因表达降低但在其他布鲁氏菌属感染中未降低的例子有生长停滞(Gas2)、免疫球蛋白受体(FcgammarI)和趋化因子受体(Cxcr4)基因,这表明对胞内功能有相反的影响。

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