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模拟太阳紫外线辐射对年轻人和老年人循环中25(OH)D3、24,25(OH)D3及其比值的影响。

The Influence of Solar-Simulated UV Radiation on Circulating 25(OH)D3, 24,25(OH)D3 and Their Ratio in Younger and Older Adults.

作者信息

Borecka Oktawia P, Tang Jonathan C Y, Fraser William D, Rhodes Lesley E, Webb Ann R

机构信息

Department of Earth and Environmental Sciences, Faculty of Science and Engineering, University of Manchester, Manchester M13 9PL, UK.

Photobiology Unit, Dermatology Research Centre, Salford Royal Hospital, Northern Care Alliance NHS Foundation Trust, Manchester Academic Health Science Centre, Manchester M6 8HD, UK.

出版信息

Nutrients. 2025 Jun 18;17(12):2039. doi: 10.3390/nu17122039.

Abstract

In addition to the well-known vitamin D metabolites 25(OH)D and 1,25(OH)D, the catabolite 24,25(OH)D may also reflect vitamin D status and influence biological and skeletal processes. However, the effects of UVR-induced synthesis on 24,25(OH)D levels and the 25-VMR (24,25(OH)D3:25(OH)D3 ratio) remain unclear. We aimed to assess how a single standardised UVR dose influences the production of 25(OH)D3, 24,25(OH)D3, 1,25(OH)D3 and 25-VMR, with a comparison between younger and older adults being conducted to explore potential age-related differences in vitamin D metabolism. : A total of 11 young (18-40 years; 7M, 4F) and 10 older (65-89 years; 6M, 4F) skin type I-III volunteers received a single sub-erythemal dose of solar simulated UVR (SSR) (95% UVA: 320-400 nm, 5% UVB: 290-320 nm, 1.3 standard erythemal dose) during winter time in the UK (vitamin D trough season), exposing approximately 35% of the body surface area. The Blood was assayed for 25(OH)D3, 24,25(OH)D3 and 1,25(OH)D3 using LC-MS/MS at baseline, 24 h and 7 days following UVR exposure. There was a significant increase in 25(OH)D3 from baseline (44 ± 22 nmoL/L) to 24 h post-UVR (48 ± 22 nmoL/L) in the combined age group ( = 0.044), but no significant differences were found in 24,25(OH)D3 in the combined group, or between young and older volunteers for both metabolites. 1,25(OH)D3 concentrations were higher in young groups (163 ± 60 pmoL/L) than in older (105 ± 38 pmoL/L) groups at 7 days post-UVR ( = 0.044). The 25-VMR decreased from baseline (9 ± 3) to 24 h post-UVR (7.5 ± 2.1) in the combined group ( = 0.003). Our data suggest that a single sub-erythemal UVR challenge does not influence 24,25(OH)D3 concentration in younger and older adults at 24 h and 7 days post-UVR and that the significant difference seen in the 25-VMR between baseline and 24 h post-UVR is due to the increase in 25(OH)D3 concentration post-UVR. This is in line with vitamin D oral supplementation studies, and indicates that low doses of UVR trigger the metabolic pathway, without affecting the catabolic pathway.

摘要

除了众所周知的维生素D代谢产物25(OH)D和1,25(OH)D外,分解代谢产物24,25(OH)D也可能反映维生素D状态,并影响生物学和骨骼过程。然而,紫外线辐射(UVR)诱导的合成对24,25(OH)D水平和25-VMR(24,25(OH)D3:25(OH)D3比值)的影响仍不清楚。我们旨在评估单次标准化UVR剂量如何影响25(OH)D3、24,25(OH)D3、1,25(OH)D3的产生以及25-VMR,并对年轻人和老年人进行比较,以探索维生素D代谢中潜在的年龄相关差异。共有11名年轻(18 - 40岁;7名男性,4名女性)和10名年长(65 - 89岁;6名男性,4名女性)的I - III型皮肤志愿者在英国冬季(维生素D低谷季节)接受了单次亚红斑剂量的太阳模拟UVR(SSR)(95% UVA:320 - 400 nm,5% UVB:290 - 320 nm,1.3标准红斑剂量),暴露约35%的身体表面积。在UVR暴露前基线、暴露后24小时和7天使用液相色谱 - 串联质谱法(LC - MS/MS)检测血液中的25(OH)D3、24,25(OH)D3和1,25(OH)D3。在合并年龄组中,25(OH)D3从基线(44±22 nmol/L)到UVR后24小时(48±22 nmol/L)有显著增加(P = 0.044),但合并组中24,25(OH)D3以及年轻和年长志愿者的这两种代谢产物之间均未发现显著差异。UVR后7天年轻组(163±60 pmol/L)的1,25(OH)D3浓度高于年长组(105±38 pmol/L)(P = 0.044)。合并组中25-VMR从基线(9±3)降至UVR后24小时(7.5±2.1)(P = 0.003)。我们的数据表明,单次亚红斑UVR刺激在UVR后24小时和7天对年轻人和老年人的24,25(OH)D3浓度没有影响,并且UVR后基线和24小时之间25-VMR的显著差异是由于UVR后25(OH)D3浓度增加所致。这与维生素D口服补充研究一致,并表明低剂量UVR触发代谢途径,而不影响分解代谢途径。

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