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锌、金属硫蛋白与长寿——补锌的影响:锌龄研究

Zinc, metallothioneins, and longevity--effect of zinc supplementation: zincage study.

作者信息

Mocchegiani Eugenio, Giacconi Robertina, Cipriano Catia, Costarelli Laura, Muti Elisa, Tesei Silvia, Giuli Cinzia, Papa Roberta, Marcellini Fiorella, Mariani Erminia, Rink Lothar, Herbein George, Varin Audrey, Fulop Tamas, Monti Daniela, Jajte Jolanta, Dedoussis George, Gonos Efstathios S, Trougakos Ioannis P, Malavolta Marco

机构信息

Immunology Center (Section: Nutrigenomic and Immunosenescence), Research Department, Italian National Research Center on Ageing, Ancona, Italy.

出版信息

Ann N Y Acad Sci. 2007 Nov;1119:129-46. doi: 10.1196/annals.1404.030.

Abstract

Aging is an inevitable biological process that is associated with gradual and spontaneous biochemical and physiological changes and increased susceptibility to diseases. Because nutritional factors are involved in improving immune functions, metabolic harmony, and antioxidant defense, some nutritional factors, such as zinc, may modify susceptibility to disease and promote healthy aging. In vitro (human lymphocytes exposed to endotoxins) and in vivo (old or young mice fed with low zinc dietary intake) studies revealed that zinc is important for immune efficiency (innate and adaptive), antioxidant activity (supeoxide dismutase), and cell differentiation via clusterin/apolipoprotein J. Intracellular zinc homeostasis is regulated by metallothioneins (MT) via ion release through the reduction of thiol groups in the MT molecule. This process is crucial in aging because high MT levels are not able to release zinc, resulting in low intracellular free ion availability for biological functions. Improvement in these functions occurs in the elderly after physiological zinc supplementation. In this study, the selection of elderly subjects for zinc supplementation is discussed in relation to the genetic background of MT and pro-inflammatory cytokines, such as interleukin-6, because the latter is involved both in MT-gene expression and in intracellular zinc homeostasis.

摘要

衰老是一个不可避免的生物学过程,与渐进性和自发性的生化及生理变化以及对疾病易感性增加相关。由于营养因素参与改善免疫功能、代谢平衡和抗氧化防御,一些营养因素,如锌,可能会改变疾病易感性并促进健康衰老。体外研究(暴露于内毒素的人类淋巴细胞)和体内研究(喂食低锌饮食的老年或幼年小鼠)表明,锌对于免疫效能(先天性和适应性)、抗氧化活性(超氧化物歧化酶)以及通过聚集素/载脂蛋白J进行的细胞分化很重要。细胞内锌稳态由金属硫蛋白(MT)通过MT分子中硫醇基团还原导致离子释放来调节。这个过程在衰老过程中至关重要,因为高水平的MT无法释放锌,导致细胞内游离离子可用于生物功能的量较低。生理补锌后老年人的这些功能会得到改善。在本研究中,结合MT和促炎细胞因子(如白细胞介素-6)的遗传背景讨论了老年受试者补锌的选择,因为后者既参与MT基因表达又参与细胞内锌稳态。

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