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Aging affects sex- and organ-specific trace element profiles in mice

机译:老化会影响小鼠中的性别和器官特定的微量元素谱

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摘要

A decline of immune responses and dynamic modulation of the redox status are observed during aging and are influenced by trace elements such as copper, iodine, iron, manganese, selenium, and zinc. So far, analytical studies have focused mainly on single trace elements. Therefore, we aimed to characterize age-specific profiles of several trace elements simultaneously in serum and organs of adult and old mice. This allows for correlating multiple trace element levels and to identify potential patterns of age-dependent alterations. In serum, copper and iodine concentrations were increased and zinc concentration was decreased in old as compared to adult mice. In parallel, decreased copper and elevated iron concentrations were observed in liver. The age-related reduction of hepatic copper levels was associated with reduced expression of copper transporters, whereas the increased hepatic iron concentrations correlated positively with proinflammatory mediators and Nrf2-induced ferritin H levels. Interestingly, the age-dependent inverse regulation of copper and iron was unique for the liver and not observed in any other organ. The physiological importance of alterations in the iron/copper ratio for liver function and the aging process needs to be addressed in further studies.
机译:在老化期间观察到免疫应答和动态调制的下降,并受铜,碘,铁,锰,硒和锌等微量元素的影响。到目前为止,分析研究主要集中在单痕量元素上。因此,我们旨在在成人和老鼠的血清和器官中表征几种微量元素的年龄特异性谱。这允许关联多个跟踪元素级别,并识别依赖于年龄依赖性变化的潜在模式。在血清中,与成虫小鼠相比,铜和碘浓度升高,锌浓度较低。在肝脏中观察到平行,铜浓度降低和升高的铁浓度。与铜转运蛋白的表达减少有关的肝铜水平的年龄相关降低,而增加的肝脏铁浓度与促炎介质和NRF2诱导的铁蛋白H水平正相关。有趣的是,铜和铁的年龄依赖性逆调节对于肝脏是独特的,并且在任何其他器官中未观察到。在进一步的研究中需要解决肝硬化/铜比的改变的生理重要性,以及在进一步的研究中进行衰老过程。

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