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首页> 外文期刊>Laboratory investigation >Phagocytosis of gadolinium chloride or zymosan induces simultaneous upregulation of hepcidin- and downregulation of hemojuvelin- and Fpn-1-gene expression in murine liver
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Phagocytosis of gadolinium chloride or zymosan induces simultaneous upregulation of hepcidin- and downregulation of hemojuvelin- and Fpn-1-gene expression in murine liver

机译:氯化g或酵母聚糖的吞噬作用会同时诱导鼠肝中hepcidin-和FH-1和Fpn-1-基因表达的上调和下调

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摘要

The liver and the spleen are the organs in which cellular material and aged erythrocytes are eliminated from the blood. Within the liver, Kupffer cells (KCs) are mainly responsible for this task, as such KCs have a pivotal role in iron metabolism. The aim of this study is to investigate the changes of hepatic gene expression in two models of KC phagocytosis. Gadolinium chloride (GD) or zymosan was injected intraperitoneally into rats and to endotoxin-resistant mice (C3H/HeJ). The animals were killed at different time points and their livers were immediately frozen in liquid nitrogen for RNA isolation and immunohistological studies. RNA was analyzed by real-time PCR and northern blot. Sera were used to measure transaminases, hepcidin and iron levels. The expression of iron metabolism genes, hepcidin, hemojuvelin (Hjv), ferroportin-1 (Fpn-1) and of the inflammatory cytokines IL-6, IL-1β, TNF-α and IFN-γ was determined. Although phagocytosed material was detected in ED-1- and C1q-positive cells, no inflammatory cells were identified within the liver parenchyma. Serum levels of hepcidin, iron and transaminases did not differ from those of control animals. Both GD and zymosan induced an upregulation of hepcidin-gene expression in rat liver as early as 3?h, reaching a maximum 6?h after treatment. Hjv- and Fpn-1-gene expression was downregulated at the same time. IL-6 was by far the most induced acute-phase-cytokine in GD- and zymosan-treated livers, although IL-1β and TNF-α were also strongly upregulated by zymosan and to a lesser extent by GD. Similar results were obtained in the C3H/HeJ mouse strain excluding the possible role of contaminating endotoxin. This study shows that phagocytosis upregulates hepcidin-gene expression and downregulates Hjv- and Fpn-1-gene expression within the liver. These changes in iron-regulating-gene expression may be mediated by the locally produced acute-phase-cytokines.
机译:肝脏和脾脏是从血液中清除细胞物质和老化的红细胞的器官。在肝脏中,枯否细胞(KCs)主要负责此任务,因为此类KC在铁代谢中起关键作用。这项研究的目的是调查两种KC吞噬模型中肝脏基因表达的变化。将氯化(GD)或zymosan腹膜内注射到大鼠和耐内毒素的小鼠(C3H / HeJ)中。在不同时间点处死动物,将其肝脏立即在液氮中冷冻以进行RNA分离和免疫组织学研究。通过实时PCR和RNA印迹分析RNA。血清用于测量转氨酶,铁调素和铁水平。测定了铁代谢基因hepcidin,hemojuvelin(Hjv),ferroportin-1(Fpn-1)以及炎性细胞因子IL-6,IL-1β,TNF-α和IFN-γ的表达。尽管在ED-1-和C1q-阳性细胞中检测到吞噬物质,但在肝实质内未发现炎性细胞。铁调素,铁和转氨酶的血清水平与对照动物无差异。 GD和zymosan均可在大鼠肝脏中最早于3?h上调Hepcidin基因的表达,在治疗后最高达到6?h。 Hjv和Fpn-1-基因表达同时下调。 IL-6是迄今为止在GD和酵母聚糖治疗的肝脏中诱导的急性期细胞因子,尽管IL-1β和TNF-α也被酵母聚糖强烈上调,而GD则有较小程度的上调。在C3H / HeJ小鼠品系中获得了相似的结果,但不包括污染内毒素的可能作用。这项研究表明,吞噬作用在肝脏中上调了hepcidin基因的表达,并下调了Hjv-和Fpn-1-基因的表达。铁调节基因表达的这些变化可能是由局部产生的急性期细胞因子介导的。

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