维生素D的增加与naïve的下降有关,但在衰老早期,效应CD8 T细胞的积累有关。

Yong Gil Hwang, Hui-Chen Hsu, Fei-Chu Lim, Qi Wu, PingAr Yang, Gordon Fisher, Gary R Hunter, John D Mountz
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引用次数: 11

摘要

鉴于25-羟基维生素D (25[OH]D或维生素D)在肌肉骨骼健康中的保护作用以及补充维生素D在降低各种慢性疾病风险方面的潜在有益作用,强化补充维生素D已被广泛提倡。值得注意的是,与其他主要免疫细胞相比,CD8 T细胞具有最高水平的维生素D受体。然而,维生素D在衰老过程中对CD8 T细胞的影响尚不清楚。本研究确定了34名健康女性(均>60岁)维生素D水平与CD8 t细胞状态之间的关系。CD8 T细胞表型由CD28和CD95的表面表达确定。低25(OH)D血清组(≤30 ng/ml) CD28+CD95-CD8+ (naïve) T细胞百分比较高,CD28+CD95+CD8+(效应)T细胞百分比较低。相比之下,25(OH)D水平高的受试者naïve CD8 T细胞的百分比非常低,但效应CD8 T细胞的百分比非常高。25(OH)D水平与naïve CD8 T细胞频率呈显著负相关。结果表明,在衰老早期,较高水平的维生素D与naïve CD8 T细胞频率降低相关,这表明较高水平的25(OH)D加速了CD8 T细胞的衰老。这些结果为进一步评估补充维生素D对免疫衰老的影响提供了依据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Increased vitamin D is associated with decline of naïve, but accumulation of effector, CD8 T cells during early aging.

Given the protective roles of 25-hydroxyvitamin D (25[OH]D or vitamin D) in musculoskeletal health and the potential beneficial effects of vitamin D supplementation in reducing the risk of various chronic diseases, intensive repletion of vitamin D has been widely advocated. Of note, CD8 T cells have the highest levels of the vitamin D receptor compared with other major immune cells. The effects of vitamin D on CD8 T cells during aging, however, remain unclear. This study determined the relationship between vitamin D levels and CD8 T-cell status in 34 healthy female subjects (all >60 years old). The CD8 T cell phenotype was defined by the surface expression of CD28 and CD95. The low-25(OH)D serum groups (≤30 ng/ml) had higher percentages of CD28+CD95-CD8+ (naïve) T cells and lower percentages of CD28+CD95+CD8+ (effector) T cells. By contrast, subjects with high levels of 25(OH)D had very low percentages of naïve CD8 T cells but very high percentages of effector CD8 T cells. There was a significant inverse correlation between 25(OH)D levels and the frequency of naïve CD8 T cells. The results show that higher levels of vitamin D are correlated with decreased frequencies of naïve CD8 T cells during early aging, suggesting that higher levels of 25(OH)D accelerate CD8 T-cell senescence. These results warrant the further evaluation of the effects of vitamin D supplementation in immune aging.

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