首页> 外文期刊>Veterinary Immunology and Immunopathology >Indices of inflammation in the lung and liver in the early stages of the black walnut extract model of equine laminitis
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Indices of inflammation in the lung and liver in the early stages of the black walnut extract model of equine laminitis

机译:马毛层炎的黑胡桃提取物模型早期肺和肝脏的炎症指标

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The liver and lung are not only described as ''target organs'' in sepsis in most species, but are purported to be sources of circulating inflammatory mediators central to the systemic inflammatory response syndrome (SIRS). As we have recently reported an inflammatory response in the laminar tissue in laminitis similar to that described in ''target organs'' in human sepsis, we investigated the inflammatory response of the lung and liver in the black walnut extract (BWE) model of equine laminitis to determine (1) if a similar systemic inflammatory response occurs in this laminitis model as described for these organs in human sepsis, and (2) if these organs may be an important source of the inflammatory mediators leading to laminar inflammation. Real-time quantitative PCR (RT-qPCR) was used to measure hepatic and pulmonary mRNA concentrations of IL-1 beta , IL-4, IL-6, IL-8, IL-10, TNF- alpha , COX-1 and COX-2. Hepatic samples were assessed from two time points in the developmental/prodromal period: (1) 1.5h post-BWE administration (BWE-1.5H, n=5), and (2) the ''developmental time point'' (onset of leukopenia, approximately 3h post-BWE administration, BWE-DEV, n=5). Pulmonary samples were only assessed for the BWE-DEV group. One control group (CON-3H, n=5) was used for both the 1.5H and DEV groups. Finally, CD13 immunohistochemistry was performed to assess leukocyte emigration into hepatic and pulmonary parenchyma. Hepatic and pulmonary mRNA concentrations of the proinflammatory cytokines IL-6, IL-8 and TNF- alpha were significantly increased (P<0.05) in BWE-1.5H and BWE-DEV groups compared to the control group; IL-1 beta mRNA concentrations were only increased in the lung. The ''anti-inflammatory'' cytokines, IL-10 and IL-4, underwent transient decreases at different time points. Significant increases in parenchymal leukocyte numbers occurred in both the lung and liver at the BWE-DEV time point. Hepatic and pulmonary proinflammatory cytokine expression differ from that previously reported for the laminae in that TNF- alpha was increased in the hepatic and pulmonary tissues, the increases in expression of IL-6 and IL-8 are dramatically smaller for the liver and lung compared to those reported for the laminae, and the peak changes appear to occur later in the disease process in the liver than in the laminae (BWE-DEV in liver vs. 1.5H in the laminae).
机译:在大多数物种中,肝和肺不仅被描述为败血症中的“靶器官”,而且据称是全身性炎症反应综合征(SIRS)的循环炎症介质的来源。正如我们最近报道的与人类败血症中“靶器官”所述的椎板炎中的层状组织炎症反应相似,我们在马黑胡桃提取物(BWE)模型中研究了肺和肝脏的炎症反应椎板炎,以确定(1)在这种椎板炎模型中是否发生了与人类败血症中这些器官类似的全身性炎症反应,以及(2)这些器官是否可能是导致层状炎症的炎性介质的重要来源。实时定量PCR(RT-qPCR)用于测量IL-1 beta,IL-4,IL-6,IL-8,IL-10,TNF-α,COX-1和COX的肝和肺mRNA浓度-2。在发育/前驱期的两个时间点评估肝样本:(1)BWE给药后1.5h(BWE-1.5H,n = 5),以及(2)“发育时间点”(发病时间为白细胞减少症,BWE治疗后约3小时,BWE-DEV,n = 5)。仅对BWE-DEV组评估了肺部样本。 1.5H和DEV组均使用一个对照组(CON-3H,n = 5)。最后,进行了CD13免疫组化评估白细胞向肝实质和肺实质的迁移。与对照组相比,BWE-1.5H和BWE-DEV组中促炎细胞因子IL-6,IL-8和TNF-α的肝和肺mRNA浓度显着增加(P <0.05); IL-1βmRNA的浓度仅在肺中增加。 “抗炎”细胞因子IL-10和IL-4在不同时间点瞬时减少。在BWE-DEV时间点,肺和肝中实质白细胞数量显着增加。肝和肺促炎细胞因子的表达与先前报道的薄层不同,在于肝和肺组织中的TNF-α升高,而肝和肺中IL-6和IL-8的表达增幅明显小于肝癌的峰值变化似乎比肝癌的发生晚于肝癌的发病过程(肝癌的BWE-DEV与肝癌的1.5H)。

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