The effect of iron dextran on vitamin D3 metabolism in SD rats

The effect of iron dextran on vitamin D3 metabolism in SD rats

Iron and vitamin D (VD) is essential to health. Previous studies have shown that iron homeostasis has a potential effect on VD metabolism, but the mechanism is not fully understood. To explore the relationship between VD metabolism and iron metabolism, as well as the regulatory mechanism of iron on...

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Veröffentlicht in:Nutrition & metabolism 2022-07, Vol.19 (1), p.1-47, Article 47
Hauptverfasser: Qiu, Fubin, Li, Rui, Gu, Siyu, Zhao, Yimin, Yang, Linxue
Format: Artikel
Sprache:eng
Schlagworte:
1,25-(OH)2D3
25-(OH)D3
Alfacalcidol
Anemia
Antibodies
Aorta
Biotechnology
Blood
Calcifediol
Calcitriol
Chloral hydrate
Correlation analysis
CYP27A1
CYP27B1
CYP2R1
Dextran
Diet
Enzymes
Erythrocytes
Health aspects
Hemoglobin
Homeostasis
Hydroxylase
Immunofluorescence
Iron
Iron deficiency
Iron-dextran complex
Kidneys
Liver
Metabolism
Nutrient deficiency
Older people
Physiological aspects
Physiology
Proteins
Serum levels
Signal transduction
Software
Stainless steel
Statistical analysis
Transferrins
Vitamin D
Vitamin D metabolism
Vitamin D3
Vitamin metabolism
Western blotting
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Zusammenfassung:Iron and vitamin D (VD) is essential to health. Previous studies have shown that iron homeostasis has a potential effect on VD metabolism, but the mechanism is not fully understood. To explore the relationship between VD metabolism and iron metabolism, as well as the regulatory mechanism of iron on VD metabolism. 40 male rats were fed adaptively for 7 days and randomly divided into control (C, n = 6 normal diet) group and model (M, n = 24 iron deficient diet) by simple randomization, the latter was used to establish iron deficiency anemia (IDA) model. After 6 weeks of feeding, the M group was randomly divided into: iron deficiency group (DFe), low iron group (LFe), medium iron group (MFe) and high iron group (HFe) by block randomization. Different doses of iron dextran (based on iron content (100 g*bw*d)): 0, 1.1, 3.3 and 9.9 mg) were given respectively. After 4 weeks, the rats were anesthetized with 8% chloral hydrate, Blood (collected from the abdominal aorta), liver and kidney tissues were collected. The serum and tissues were separately packed and frozen at -80â for testing. The results showed that the levels of hemoglobin (Hb), red blood cell (RBC), serum iron (SI), liver iron, and kidney iron in DFe group were lower than those in the other four groups, while the levels of total iron-binding capacity (TIBC), transferrin (TF) and transferrin receptor (Tfr) in DFe group were higher than those in other groups; The serum levels of 25-(OH)D.sub.3 and 1,25-(OH).sub.2D.sub.3 in DFe group were significantly lower than those in C group (P < 0.05). The correlation analysis showed that the levels of 25-(OH)D.sub.3 and 1,25-(OH).sub.2D.sub.3 were negatively correlated with TIBC, TF and Tfr no correlation with SI. Western blotting, immunofluorescence, and q-PCR results showed that compared with C group, the protein and gene expressions of CYP2R1, CYP27A1, and CYP24A1 in DFe group were down-regulated, and the expression of CYP27B1 protein and gene was up-regulated in DFe group. Iron may be involved in the metabolism of VD.sub.3 by regulating the expression of VD.sub.3 hydroxylase, suggesting that appropriate iron supplementation might promote the activation of VD.sub.3.
ISSN:1743-7075
1743-7075
DOI:10.1186/s12986-022-00681-5