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首页> 外文期刊>Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology >Newly recruited human monocytes have a preserved responsiveness towards bacterial peptides in terms of CD11b up-regulation and intracellular hydrogen peroxide production.
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Newly recruited human monocytes have a preserved responsiveness towards bacterial peptides in terms of CD11b up-regulation and intracellular hydrogen peroxide production.

机译:就CD11b的上调和细胞内过氧化氢的产生而言,新招募的人类单核细胞对细菌肽的反应性得以保留。

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The transmigration of peripheral human monocytes to the interstitium is a fundamental step in the host-defence mechanism against infections. Little is known about the state of function of in vivo transmigrated interstitial monocytes prior to differentiation into macrophages and dendritic cells. We hypothesized that newly recruited interstitial monocytes have a preserved responsiveness against bacterial-related peptides, giving them a specific role in the immediate defence against invading pathogens. In order to test this hypothesis, we explored the responsiveness of in vivo transmigrated as well as peripheral monocytes, in terms of CD11b expression and H(2)O(2) production towards the bacterial-related peptide formylmethionylleucylphenylalanine (fMLP) by the use of a skin chamber technique. In addition, we analysed the concentration of interleukin (IL)-8, monocyte chemotactic protein-1 (MCP-1) and tumour necrosis factor (TNF)-alpha in the skin blister exudates and in the circulation. We demonstrate thatin vivo-transmigrated monocytes had a fivefold higher CD11b expression compared to monocytes obtained from the peripheral circulation. fMLP exposure induced a significantly higher CD11b expression on transmigrated cells compared to peripheral monocytes. In addition, newly recruited monocytes had a preserved H(2)O(2) production. The interstitial concentration of IL-8, MCP-1 and TNF-alpha was significantly higher in blister exudates compared to that in the peripheral circulation. Thus, in vivo transmigrated human monocytes preserve their capacity to respond towards bacterial peptides in terms of CD11b up-regulation and H(2)O(2) generation. These data strengthen a role for newly recruited interstitial human monocytes in the immediate defence against invading pathogens.
机译:外周人类单核细胞向间质的迁移是抵抗感染的宿主防御机制中的基本步骤。关于体内迁移的间质单核细胞在分化为巨噬细胞和树突状细胞之前的功能状态知之甚少。我们假设,新募集的间质单核细胞对细菌相关肽具有保留的响应性,从而在立即防御入侵的病原体方面发挥了特定作用。为了检验此假设,我们通过使用CD11b表达和H(2)O(2)对细菌相关肽甲酰甲硫基亮氨酰苯丙氨酸(fMLP)的产生,探讨了体内迁移的以及外周单核细胞的反应性。皮肤室技术。此外,我们分析了皮肤水疱渗出液和循环系统中白介素(IL)-8,单核细胞趋化蛋白1(MCP-1)和肿瘤坏死因子(TNF)-α的浓度。我们证明体内迁移的单核细胞与从外周循环获得的单核细胞相比具有更高的CD11b表达五倍。与外周单核细胞相比,fMLP暴露在移行细胞上诱导了更高的CD11b表达。此外,新招募的单核细胞具有保存的H(2)O(2)生产。与周围循环相比,水疱渗出液中IL-8,MCP-1和TNF-α的间质浓度明显更高。因此,体内迁移的人类单核细胞保留了它们对CD11b上调和H(2)O(2)生成的细菌肽作出反应的能力。这些数据增强了新募集的间质人单核细胞在立即防御入侵病原体方面的作用。

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