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Differential Responses to Vitamin D2 and Vitamin D3 Are Associated With Variations in Free 25-Hydroxyvitamin D

机译:维生素D2和维生素D3的差异反应与游离25-羟基维生素D的变化有关

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摘要

25-Hydroxyvitamin D (25D) circulates bound primarily to serum vitamin D binding protein (DBP), with DBP showing higher binding affinity for 25D3 than 25D2. We therefore hypothesized that vitamin D2 (D2) promotes higher serum levels of unbound 25D (free 25D), with different functional responses, relative to vitamin D3 (D3). Week 3 C56BL/6 mice were placed on diets containing either D2 or D3 alone (both 1000 IU/kg). At week 8 and week 16, D2 mice had only 25D2 in circulation (26.6 ± 1.9 and 33.3 ± 4.4 ng/mL), and D3 mice had only 25D3 (28.3 ± 2.0 and 31.7 ± 2.1 ng/mL). At week 8 (44.5 ± 6.4 vs 62.4 ± 11.6 pg/mL, P < .05) and week 16 (78.4 ± 12.6 vs 95.5 ± 11.6), D2 mice had lower serum 1,25-dihydroxyvitamin D relative to D3 mice. By contrast, measured free 25D was significantly higher in D2 mice at week 8 (16.8 ± 0.65 vs 8.4 ± 0.63 pg/mL, P < .001) and week 16 (17.4 ± 0.43 vs 8.4 ± 0.44, P < .001). A two-way ANOVA of bone histomorphometry showed that week 8 D2 mice had significantly higher osteoclast surface/bone surface, eroded surface/bone surface, and mineral apposition rate compared with D3 mice. Osteoblast surface/bone surface was higher in week 8 D2 females but not week 8 D2 males. At week 16, D2 mice had significantly higher bone volume/total volume and trabecular number compared with D3 mice. Differences in bone phenotype were observed despite D2 mice reaching similar serum 25D levels and lower 1,25D levels compared with D3 mice. These data indicate that 25D2 binds less well to DBP than 25D3, with resulting higher levels of free 25D promoting differential effects on bone in mice exposed to D2 alone.
机译:25-羟基维生素D(25D)主要与血清维生素D结合蛋白(DBP)结合循环,与25D2相比,DBP对25D3的结合亲和力更高。因此,我们假设相对于维生素D3(D3),维生素D2(D2)促进未结合的25D(游离25D)的血清水平更高,具有不同的功能响应。将第3周的C56BL / 6小鼠置于单独含有D2或D3(均为1000 IU / kg)的饮食中。在第8周和第16周,D2小鼠的循环中只有25D2(26.6±1.9和33.3±4.4 ng / mL),D3小鼠只有25D3(28.3±2.0和31.7±2.1 ng / mL)。在第8周(44.5±6.4对62.4±11.6 pg / mL,P <.05)和第16周(78.4±12.6对95.5±11.6),D2小鼠的血清1,25-二羟基维生素D相对于D3小鼠较低。相比之下,D2小鼠在第8周(16.8±0.65 vs 8.4±0.63 pg / mL,P <.001)和第16周(17.4±0.43 vs 8.4±0.44,P <.001)时,测得的游离25D显着更高。骨组织形态计量学的双向ANOVA显示,与D3小鼠相比,第8周D2小鼠的破骨细胞表面/骨表面,侵蚀的表面/骨表面和矿物质附着率显着更高。 8周D2雌性中成骨细胞表面/骨表面较高,而8周D2雄性中成骨表面/骨表面较高。在第16周,与D3小鼠相比,D2小鼠的骨体积/总体积和小梁数目明显更高。尽管与D3小鼠相比D2小鼠达到相似的血清25D水平和更低的1,25D水平,但仍观察到骨表型差异。这些数据表明25D2与DBP的结合要比25D3少,从而导致较高水平的游离25D促进单独暴露于D2的小鼠对骨骼的差异作用。

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