Effect of oral vitamin C on serum hepcidin level, iron status and inflammation among hemodialysis patients with functional iron deficiency anaemia

M. Behairy, A. Gharib, M. Zaki, Reem El Sharabasy
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Abstract

Introduction: Hepcidin is a key regulatory peptide in iron homeostasis, the pathogenesis of functional iron deficiency (FID) anemia and erythropoiesis-stimulating agent (ESA) resistance is contributed to the inflammatory mediated increase in the serum hepcidin levels among prevalent hemodialysis (HD) patients. Objectives: To test the reducing therapeutic effect of oral vitamin C supplements on hepcidin levels and iron status among HD patients with FID anemia. Patients and Methods: This study is an interventional prospective cohort study; 48 prevalent HD patients were enrolled. Group one: 31 patients who received the conventional treatment of erythropoietin stimulating agents together with oral supplementation of vitamin C 500 mg every other day dose for 3 months. Group two: 17 patients who received only the conventional therapy of erythropoietin stimulating agents. Patients with hemoglobin level <11 g/dL, ferritin level >200 ng/mL and transferrin saturation (TSAT) >20 % were included. Laboratory parameters: serum hepcidin, high-sensitivity C-reactive protein (hs-CRP) titre, CBC, and iron indices were measured at baseline and after 3 months. Results: On comparing the two groups, oral vitamin C in group 1 resulted in a statistically significant reduction in hepcidin levels [mean 2506.456 ± 1320.53 pg/mL to 1748.396 ± 1432.28 pg/mL (P = 0.03)], and a significant reduction in hs-CRP level [mean 8603.236 ± 2547.77 ng/mL to 5611.296 ± 2829.27 ng/mL] (P = 0.001) after three months of treatment in comparison to control group. A decrease of EPO requirement and elevation of hemoglobin level were observed in a study group with oral vitamin C. Conclusion: Oral vitamin C may be a promising therapy in decreasing serum hepcidin and inflammatory markers among prevalent HD patients with FID anemia.
口服维生素C对功能性缺铁性贫血血液透析患者血清hepcidin水平、铁状态及炎症的影响
Hepcidin是铁稳态的关键调节肽,在血透(HD)患者中,功能性缺铁(FID)贫血和促红细胞生成素(ESA)抵抗的发病机制与炎症介导的血清Hepcidin水平升高有关。目的:探讨口服维生素C补充剂对HD合并FID贫血患者hepcidin水平和铁状态的降低治疗作用。患者和方法:本研究是一项干预性前瞻性队列研究;纳入了48例流行的HD患者。第一组:31例患者,给予常规促红细胞生成素药物治疗,同时口服维生素C 500 mg,每隔一天给药,疗程3个月。第二组:仅给予促红细胞生成素常规治疗的17例。纳入血红蛋白水平200 ng/mL、转铁蛋白饱和度(TSAT) > 20%的患者。实验室参数:在基线和3个月后测定血清hepcidin、高敏c反应蛋白(hs-CRP)滴度、CBC、铁指标。结果:两组比较,口服维生素C组治疗3个月后hepcidin水平[平均2506.456±1320.53 pg/mL至1748.396±1432.28 pg/mL (P = 0.03)]和hs-CRP水平[平均8603.236±2547.77 ng/mL至5611.296±2829.27 ng/mL]较对照组显著降低(P = 0.001)。结论:口服维生素C可能是一种很有希望的治疗方法,可以降低流行的HD合并FID贫血患者的血清hepcidin和炎症标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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