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首页> 外文期刊>Proteomics >The cellular and proteomic response of primary and immortalized murine Kupffer cells following immune stimulation diverges from that of monocyte-derived macrophages
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The cellular and proteomic response of primary and immortalized murine Kupffer cells following immune stimulation diverges from that of monocyte-derived macrophages

机译:免疫刺激后原代和永生化鼠Kupffer细胞的细胞和蛋白质组学反应与单核细胞衍生的巨噬细胞不同

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Kupffer cells (KCs) are the first line of defense in the liver against pathogens, yet several microbes successfully target the liver, bypass immune surveillance, and effectively develop in this tissue. Our current, albeit poor, understanding of KC-pathogen interactions has been largely achieved through the study of primary cells, requiring isolation from large numbers of animals. To facilitate the study of KC biology, an immortalized rat KC line 1, RKC1, was developed. We performed a comparative global proteomic analysis of RKC1 and primary rat KCs (PRKC) to characterize their respective responses to lipopolysaccharide-mediated immune stimulation. We identified patent differences in the proteomic response profile of RKC1 and PRKC to lipopolysaccharide. We observed that PRKC upregulated more immune function pathways and exhibited marked changes in cellular morphology following stimulation. We consequently analyzed the cytoskeletal signaling pathways of these cells in light of the fact that macrophages are known to induce cytoskeletal changes in response to pathogens. Our findings suggest that KCs respond differently to inflammatory stimulus than do monocyte-derived macrophages, and such data may provide insight into how pathogens, such as the malaria parasite, may have evolved mechanisms of liver entry through KCs without detection.
机译:Kupffer细胞(KCs)是肝脏抵御病原体的第一道防线,但仍有几种微生物成功靶向肝脏,绕过了免疫监视,并在该组织中有效发育。通过对原代细胞的研究,我们目前对KC-病原体相互作用的了解虽然很差,但仍需要大量动物的分离。为了促进对KC生物学的研究,开发了永生的大鼠KC系1 RKC1。我们对RKC1和原代大鼠KC(PRKC)进行了比较全球蛋白质组学分析,以表征它们各自对脂多糖介导的免疫刺激的反应。我们在RKC1和PRKC对脂多糖的蛋白质组学反应中发现了专利差异。我们观察到PRKC上调了更多的免疫功能途径,并在刺激后表现出细胞形态的显着变化。因此,鉴于已知巨噬细胞诱导对病原体的反应而引起细胞骨架变化的事实,我们分析了这些细胞的细胞骨架信号通路。我们的发现表明,与单核细胞衍生的巨噬细胞相比,KC对炎症刺激的反应不同,这些数据可以提供对病原体(例如疟原虫)如何通过KC进入肝脏的机制的深入了解而无法发现。

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