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首页> 外文期刊>Mechanisms of Ageing and Development >Interrelationships among brain, endocrine and immune response in ageing and successful ageing: role of metallothionein III isoform.
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Interrelationships among brain, endocrine and immune response in ageing and successful ageing: role of metallothionein III isoform.

机译:衰老和成功衰老过程中大脑,内分泌和免疫反应之间的相互关系:金属硫蛋白III同工型的作用。

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摘要

Metallothionein-III (MT-III) a brain-specific member of metallothionein family contributes to zinc neuronal homeostasis, and zinc is an important regulator of many brain functions, including the activity of hormone realising factors by hippocampus. Among them, somatostatin is pivotal because affecting thyroid hormones turnover and consequently thymic and peripheral immune efficiency (Natural Killer, NK) cell activity. Somatostatin is in turn affected by somatomedin-C, which is also zinc-dependent. Therefore, somatomedin-C may be a marker of somatostatin status in the hippocampus. MTs sequester and release zinc in transient stress, as it may occur in young age, to protect cells by reactive oxygen species. In order to accomplish this task, MTs are induced by IL-6 for a prompt immune and anti-inflammatory response. During ageing, MTs are high with a role of sequester of zinc, but with very limited role in zinc release because stress-like condition and inflammation is persistent. Therefore, high MTs may become to protective in young age to harmful during ageing leading to low zinc ion bioavailability for many body homeostatic mechanisms, including brain function. As a consequence, an altered physiological cascade from the brain (upstream) to endocrine and immune system (downstream) may occur. The aim of this work is to study the role of MT-III in the interrelationships among brain-endocrine-immune response in ageing and successful ageing. The main results are: (1) MT-III and IL-6 gene expressions increase in the hippocampus from old mice, in comparison with young and very old mice. (2) Somatomedin-C plasma levels decrease in old mice in comparison with young and very old mice. (3) Low zinc ion bioavailability (tested by the ratio total thymulin/active thymulin) is coupled with altered thyroid hormone turnover and depressed IL-2 in old mice in comparison with young and very old mice. (4) 'In vitro' experiments display more increments on NK cells activity by adding zinc-bound active thymulin than T3 alone. In conclusion, low MT-III in the hippocampus from young and very old mice leads to good zinc ion bioavailability that it is upstream coupled with normal hippocampal function affecting downstream normal thyroid hormones turnover and satisfactory NK cell activity, via complete saturation of zinc-bound active thymulin molecules. Therefore, a correct MTs homeostasis is pivotal for brain-endocrine-immune response in order to reach successful ageing.
机译:金属硫蛋白-III(MT-III)是金属硫蛋白家族的大脑特定成员,有助于锌神经元的稳态,锌是许多脑功能的重要调节剂,包括海马体激素实现因子的活性。其中,生长抑素至关重要,因为它会影响甲状腺激素的转换,进而影响胸腺和外周免疫效率(Natural Killer,NK)的细胞活性。生长抑素又受生长激素-C(也依赖锌)的影响。因此,生长抑素C可能是海马生长抑素状态的标志。 MT会在短暂的应力中螯合并释放锌,因为锌可能会在年轻时出现,以通过活性氧来保护细胞。为了完成此任务,IL-6诱导MT产生迅速的免疫和抗炎反应。在老龄化期间,MT较高,具有螯合锌的作用,但在锌释放中的作用非常有限,因为类似应激的状况和炎症持续存在。因此,高MTs可能会在年轻时起到保护作用,在衰老过程中对人体有害,从而导致许多人体稳态机制(包括脑功能)的锌离子生物利用度降低。结果,可能发生从大脑(上游)到内分泌和免疫系统(下游)的生理级联改变。这项工作的目的是研究MT-III在衰老和成功衰老中脑内分泌免疫反应之间的相互关系中的作用。主要结果是:(1)与年幼和非常年老的小鼠相比,年老的小鼠海马中MT-III和IL-6基因表达增加。 (2)与年幼和非常年老的小鼠相比,年老小鼠的生长激素-C血浆水平降低。 (3)与年老和年纪较大的小鼠相比,老年小鼠的锌离子生物利用度低(通过总胸腺素/活性胸腺素之比测试)与甲状腺激素转换改变和IL-2降低有关。 (4)“体外”实验显示,与单独的T3相比,通过添加锌结合的活性百里香素,NK细胞的活性增加更多。总之,幼鼠和非常老的小鼠海马中的MT-III含量较低,会导致锌离子的生物利用度较高,即上游结合海马功能正常,从而影响下游正常甲状腺激素的转化,并通过锌结合完全饱和而影响令人满意的NK细胞活性。活性百里香素分子。因此,正确的MT稳态对于大脑内分泌免疫反应至关重要,以达到成功的衰老。

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