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(Healthy) Ageing: Focus on Iodothyronines

机译:(健康)衰老:专注于碘甲状腺素

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The activity of the thyroid gland diminishes during ageing, but a certain tissue reserve of T3 and its metabolites is maintained. This reserve is thought to play a regulatory role in energy homeostasis during ageing. This review critically assesses this notion. T3 was thought to act predominantly through pathways that require transcriptional regulation by thyroid hormone receptors (TRs). However, in recent years, it has emerged that T3 and its metabolites can also act through non-genomic mechanisms, including cytosolic signaling. Interestingly, differences may exist in the non-genomic pathways utilized by thyroid hormone metabolites and T3. For instance, one particular thyroid hormone metabolite, namely 3,5-diiodo-l-thyronine (T2), increases the activity of the redox-sensitive protein deacetylase SIRT1, which has been associated with improvements in healthy ageing, whereas evidence exists that T3 may have the opposite effect. Findings suggesting that T3, T2, and their signaling pathways, such as those involving SIRT1 and AMP-activated protein kinase (AMPK), are associated with improvements in diet-induced obesity and insulin resistance emphasize the potential importance of the thyroid during ageing and in ageing-associated metabolic diseases.
机译:甲状腺的活性在衰老过程中会减少,但仍保留一定的T3组织及其代谢产物。人们认为该储备在衰老过程中对能量稳态具有调节作用。这篇评论严格地评估了这个概念。 T3被认为主要通过需要甲状腺激素受体(TRs)转录调控的途径起作用。然而,近年来,已经发现T3及其代谢物也可以通过非基因组机制起作用,包括胞浆信号传导。有趣的是,甲状腺激素代谢产物和T3利用的非基因组途径可能存在差异。例如,一种特定的甲状腺激素代谢物,即3,5-二碘-1-胸腺嘧啶(T2),增加了氧化还原敏感蛋白脱乙酰基酶SIRT1的活性,这与健康衰老的改善有关,而有证据表明T3可能有相反的效果。研究结果表明,T3,T2及其信号传导途径(如涉及SIRT1和AMP激活的蛋白激酶(AMPK)的途径)与饮食诱导的肥胖症和胰岛素抵抗的改善相关,这突出了甲状腺在衰老过程中的潜在重要性。与衰老相关的代谢性疾病。

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