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脂多糖输注上调马肝中铁调素 mRNA 的表达。

Lipopolysaccharide infusion up-regulates hepcidin mRNA expression in equine liver.

机构信息

Department of Veterinary Clinical Science, School of Veterinary Medicine and Animal Science, UNESP - Univ Estadual Paulista, Botucatu, Brazil.

出版信息

Innate Immun. 2012 Jun;18(3):438-46. doi: 10.1177/1753425911420181. Epub 2011 Sep 16.

DOI:10.1177/1753425911420181
PMID:21926164
Abstract

Hepcidin has been found to be the key regulator of iron metabolism that leads to hypoferremia during inflammation. Recent work has shown that equine hepcidin is predominantly expressed in the liver of horses. In this study, hepcidin gene expression was determined in the liver and bone marrow of six healthy horses after iv infusion of Escherichia coli O55:B5 LPS. The IL-6 gene expression was also determined in liver and bone marrow samples. Clinical and laboratory evaluations were measured at multiple time points between 0 and 240 h post-LPS infusion (PI). Liver and bone marrow biopsies were taken immediately before (baseline) and at 6 and 18 h PI. In response to endotoxin infusion, all horses showed characteristic clinical signs of endotoxemia. Plasma iron concentration was decreased significantly from the pre-infusion level at 8 h PI. Hypoferremia peak was observed at 12 h and returned to normal levels at 30 h PI. Relative real-time RT-PCR analysis showed that liver hepcidin and IL-6 mRNA expression was up-regulated at 6 h PI. Bone marrow hepcidin relative expression was not influenced by LPS infusion. In another experiment, equine monocyte cultures were stimulated with LPS (1 µg/ml). Monocyte hepcidin and IL-6 gene expression was significantly induced after 2 h of LPS stimulus and returned to baseline levels thereafter. The present study describes that, in horses, LPS infusion up-regulates hepatic hepcidin mRNA expression resulting in early observed hypoferremia and suggests that hepcidin may act as an acute-phase protein in horses.

摘要

铁调素已被发现是铁代谢的关键调节剂,可导致炎症期间的低铁血症。最近的研究表明,马的铁调素主要在肝脏中表达。在这项研究中,在静脉内输注大肠杆菌 O55:B5 LPS 后,测定了 6 匹健康马的肝脏和骨髓中的铁调素基因表达。还测定了肝和骨髓样本中的 IL-6 基因表达。在 LPS 输注后(PI)的 0 至 240 小时之间的多个时间点测量临床和实验室评估。在 PI 前(基线)和 6 小时和 18 小时进行肝和骨髓活检。在对内毒素输注的反应中,所有马均表现出内毒素血症的特征性临床症状。从 PI 前的铁浓度在 8 小时时显着降低。低铁血症峰值在 12 小时时观察到,在 30 小时时恢复正常水平。相对实时 RT-PCR 分析表明,肝铁调素和 IL-6 mRNA 表达在 PI 6 小时时上调。LPS 输注对骨髓铁调素相对表达没有影响。在另一个实验中,用 LPS(1μg/ml)刺激马单核细胞培养物。LPS 刺激后 2 小时单核细胞铁调素和 IL-6 基因表达显着诱导,并随后恢复到基线水平。本研究表明,在马中,LPS 输注上调肝铁调素 mRNA 表达导致早期观察到的低铁血症,并表明铁调素可能在马中作为急性期蛋白发挥作用。

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