The correlation between hepcidin levels and iron parameters in patients with end-stage renal disease on regular hemodialysis successfully treated from hepatitis C virus by directly acting antiretrovirals

Magdy El Sharkawy, H. E. El Said, M. Behairy, F. Ahmed, Mohamed Sharaf, L. Khedr
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Abstract

Background Hepcidin is a polypeptide secreted from the liver. It regulates iron metabolism by blocking further iron absorption when iron stores are high. Hepcidin levels are usually higher than the normal range in hemodialysis (HD) patients. Hepatitis C virus (HCV) infection leads to lowering of hepcidin levels, leading to more iron overload. The objectives were to determine whether there is a correlation between iron stores and hepcidin levels in HD patients after HCV treatment and to assess the level of hepcidin in those patients who were treated from HCV compared with those who have chronic HCV infection. Patients and methods In total, 60 patients on regular HD were recruited and 30 healthy controls . Group I: 30 patients who have been successfully treated from HCV by directly acting antiretroviral drugs with a persistently negative PCR for at least 3 months, group II: 30 patients with chronic HCV infection, and 30 healthy controls form group III. Serum hepcidin levels, iron profile, and complete blood count were compared in all groups. Results Hepcidin levels were significantly higher in the HCV-treated group versus the HCV-infected group (mean 226.77±144.13 and 87.77±40.77 ng/dl), respectively, significantly higher transferrin-binding capacity (TIBC), and mean levels 410.5±74.65 and 310.93±122.57 μg/dl . Ferritin levels were higher in the HCV-infected group (355.13±196, 899.5±1522 ng/dl) than in HCV-treated. There was a significant correlation between hepcidin and serum iron, TIBC, and transferrin saturation in the HCV-treated group. On regression analysis, only TIBC and transferrin saturation correlated significantly. Conclusions Post HCV treatment with directly acting antiretroviral drugs, hepcidin levels are higher than during HCV-infection state and correlate significantly to higher TIBC . Further studies are needed to establish the effect of iron supplementation on hepcidin level in this subgroup of patients.
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直接作用抗逆转录病毒药物治疗丙型肝炎成功的终末期肾脏疾病定期血液透析患者hepcidin水平与铁参数的相关性
肝磷脂是一种由肝脏分泌的多肽。当铁储量高时,它通过阻止铁的进一步吸收来调节铁的代谢。血液透析(HD)患者的Hepcidin水平通常高于正常范围。丙型肝炎病毒(HCV)感染导致hepcidin水平降低,导致更多的铁超载。目的是确定HCV治疗后HD患者的铁储量和hepcidin水平之间是否存在相关性,并评估HCV治疗患者与慢性HCV感染患者的hepcidin水平。患者和方法共招募60例常规HD患者和30例健康对照。第一组:30名通过直接作用抗逆转录病毒药物成功治疗HCV且PCR持续阴性至少3个月的患者;第二组:30名慢性HCV感染患者和30名健康对照者组成第三组。比较各组血清hepcidin水平、铁谱和全血细胞计数。结果hcv治疗组Hepcidin水平显著高于hcv感染组(平均226.77±144.13和87.77±40.77 ng/dl),转铁蛋白结合能力(TIBC)显著高于hcv感染组(平均410.5±74.65和310.93±122.57 μg/dl)。hcv感染组的铁蛋白水平(355.13±196,899.5±1522 ng/dl)高于hcv治疗组。hcv治疗组hepcidin与血清铁、TIBC和转铁蛋白饱和度有显著相关性。在回归分析中,只有TIBC与转铁蛋白饱和度显著相关。结论丙型肝炎病毒直接抗逆转录病毒药物治疗后,hepcidin水平高于丙型肝炎病毒感染状态,并与较高的TIBC显著相关。需要进一步的研究来确定铁补充对该亚组患者hepcidin水平的影响。
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