Beijing Chao-Yang Hospital, Capital Medical University, No.8 Gongti South Road, Chaoyang District, Beijing, 100020, PR China.
Beijing Chao-Yang Hospital, Capital Medical University, No.8 Gongti South Road, Chaoyang District, Beijing, 100020, PR China.
J Steroid Biochem Mol Biol. 2023 May;229:106250. doi: 10.1016/j.jsbmb.2023.106250. Epub 2023 Jan 25.
Vitamin D is a steroid hormone precursor that was initially recognized for its important roles in calcium-phosphate homeostasis and bone health. However, the resent prevalence of vitamin D deficiency has highlighted its non-skeletal function, such as its important role in regulating endogenous metabolism. The aim of the present study was to examine the roles of vitamin D supplementation or deficiency on metabolic phenotypes in both male and female mice by using targeted metabolomics analysis. Six weeks old C57BL/6 mice of different sexes were fed with standard chow diet (1000 IU/kg vitamin D3 contained), vitamin D deficient diet (0 IU/kg vitamin D3 contained), or vitamin D enriched diet (10,000 IU/kg vitamin D3 contained) for a total of 14 weeks. Liver pathological analysis showed that vitamin D deficiency caused significant fat deposition in both male and female mice. While vitamin D supplementation was found to improve the accumulation of fat in the liver tissue. Metabolomics analysis indicated that metabolic perturbation related to vitamin D regulation in male mice mainly involved in tricarboxylic acid cycle, fatty acylcarnitine and fatty acid metabolism, sugar metabolism, glutathione metabolism, steroid hormone and pyrimidine metabolism. Based on the criteria of VIP> 1 in OPLS-DA analysis and P < 0.05 in hypothesis test, a total of 62 metabolites and 78 metabolites were found to be significantly changed in VD-deficiency group and VD-supplement group compared with the control group, respectively. While for female mice, the metabolites disturbance mainly involved in fatty acylcarnitine and fatty acid metabolism, TCA, sugar metabolism, folate cycle, methionine cycle, and purine metabolism. A total of 38 and 57 metabolites were found to be significantly changed (VIP>1 and P < 0.05) in VD-deficiency group and VD-supplement group compared with the control group, respectively. Energy metabolism was the most relevant metabolic pathway for vitamin D regulation in both male and female mice. Sex-specific changes of fatty acyl carnitines and dehydroepiandrosterone were observed in the vitamin D supplementation groups. However, most of the energy metabolism related compounds exhibited the same trend in vitamin D supplementation groups of different sexes. Pearson's correlation analysis indicated that vitamin D was significantly correlated (P < 0.05) with the levels of D-fructose 6-phosphate, D-glucose 1-phosphate, D-glucose 6-phosphate, DL-pyroglutamic acid, 2-oxoglutarate, L-glutamic acid, and fumarate, which were all involved in the sugar metabolism pathway. The results achieved in this study demonstrated that vitamin D significantly regulated the metabolism of lipid and sugar, and the regulation showed a certain sex specificity.
维生素 D 是一种类固醇激素前体,最初因其在钙磷稳态和骨骼健康中的重要作用而被认识。然而,最近维生素 D 缺乏症的流行凸显了其非骨骼功能,如在调节内源性代谢中的重要作用。本研究的目的是通过靶向代谢组学分析,研究维生素 D 补充或缺乏对雄性和雌性小鼠代谢表型的影响。不同性别的 6 周龄 C57BL/6 小鼠分别用标准饲料(含 1000 IU/kg 维生素 D3)、维生素 D 缺乏饲料(不含维生素 D3)或维生素 D 丰富饲料(含 10000 IU/kg 维生素 D3)喂养 14 周。肝脏病理分析表明,维生素 D 缺乏导致雌雄小鼠肝脏脂肪沉积明显。而维生素 D 补充被发现可改善肝脏组织中脂肪的堆积。代谢组学分析表明,与维生素 D 调节相关的代谢紊乱主要涉及三羧酸循环、脂肪酸酰基辅酶 A 和脂肪酸代谢、糖代谢、谷胱甘肽代谢、甾体激素和嘧啶代谢。根据 OPLS-DA 分析中 VIP>1 和假设检验中 P<0.05 的标准,与对照组相比,VD 缺乏组和 VD 补充组分别有 62 种和 78 种代谢物显著变化。而对于雌性小鼠,代谢物的紊乱主要涉及脂肪酸酰基辅酶 A 和脂肪酸代谢、TCA、糖代谢、叶酸循环、蛋氨酸循环和嘌呤代谢。与对照组相比,VD 缺乏组和 VD 补充组分别有 38 种和 57 种代谢物(VIP>1 和 P<0.05)显著变化。能量代谢是维生素 D 调节雄性和雌性小鼠代谢的最相关代谢途径。在维生素 D 补充组中观察到雄性和雌性小鼠的脂肪酸酰基辅酶 A 和脱氢表雄酮有性别特异性变化。然而,不同性别维生素 D 补充组的大多数与能量代谢相关的化合物表现出相同的趋势。Pearson 相关性分析表明,维生素 D 与 D-果糖 6-磷酸、D-葡萄糖 1-磷酸、D-葡萄糖 6-磷酸、DL-吡咯谷氨酸、2-氧戊二酸、L-谷氨酸和延胡索酸的水平显著相关(P<0.05),这些化合物均参与糖代谢途径。本研究结果表明,维生素 D 显著调节脂质和糖的代谢,且这种调节具有一定的性别特异性。
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