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首页> 外文期刊>Journal of proteomics >Differential proteomics reveals age-dependent liver oxidative costs of innate immune activation in mice
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Differential proteomics reveals age-dependent liver oxidative costs of innate immune activation in mice

机译:差异蛋白质组学揭示了小鼠固有免疫激活的年龄依赖性肝脏氧化成本

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摘要

Individual response to an immune challenge results from the optimization of a trade-off between benefits and costs of immune cell activation. Age-related immune disorders may have several mechanistic bases, from immune cell defects to chronic pro-inflammatory status and oxidative imbalance, but we are still lacking experimental data showing the relative importance of each of these mechanisms. Using a proteomic approach and subsequent biochemical validations of proteomics-derived hypotheses, we found age-dependent regulations in the liver of 3-months and 1-year old-mice in response to an acute innate immune activation. Old mice presented a chronic up-regulation of several proteins involved in pathways related to oxidative stress control. Interestingly, these pathways were weakly affected by the innate immune activation in old compared to young individuals. In addition, old mice suffered from lower glutathione-S-transferase activity and from higher oxidative damage at the end of the experiment, thus suggesting that they paid a higher immune-related cost than young individuals. On the whole, our data showed that a substantial fraction of the liver costs elicited by an activation of the innate immune response is effectively related to oxidative stress, and that ageing impairs the capacity of old individuals to control it.
机译:对免疫挑战的个体反应源于免疫细胞激活的收益与成本之间的折衷优化。与年龄相关的免疫疾病可能具有多种机制基础,从免疫细胞缺陷到慢性促炎状态和氧化失衡,但我们仍然缺乏实验数据来表明每种机制的相对重要性。使用蛋白质组学方法和随后的蛋白质组学假设的生化验证,我们发现3个月龄和1岁大小鼠的肝脏对急性先天免疫激活反应具有年龄依赖性。老年小鼠呈现出与氧化应激控制相关途径中涉及的几种蛋白质的慢性上调。有趣的是,与年轻人相比,老年人的先天免疫激活对这些途径的影响微弱。另外,在实验结束时,老年小鼠的谷胱甘肽-S-转移酶活性较低,且氧化损伤较高,因此表明它们的免疫相关成本要高于年轻个体。总体而言,我们的数据表明,先天免疫反应的激活所引起的肝脏费用的很大一部分与氧化应激有效相关,并且衰老削弱了老年人控制它的能力。

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