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Inverse Relationship of Serum Hepcidin Levels with CD4 Cell Counts in HIV-Infected Patients Selected from an Indonesian Prospective Cohort Study

机译:从印度尼西亚前瞻性队列研究中选择的HIV感染患者的血清铁调素水平与CD4细胞计数成反比

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摘要

BACKGROUND: Distortion of iron homeostasis may contribute to the pathogenesis of human immunodeficiency virus (HIV) infection and tuberculosis (TB). We studied the association of the central iron-regulatory hormone hepcidin with the severity of HIV and the association between hepcidin and other markers of iron homeostasis with development of TB. METHODS: Three groups of patients were selected from a prospective cohort of HIV-infected subjects in Bandung, Indonesia. The first group consisted of HIV-infected patients who started TB treatment more than 30 days after cohort enrollment (cases). The second group consisted of HIV-infected patients who were matched for age, gender and CD4 cell count to the cases group (matched controls). The third group consisted of HIV-infected patients with CD4 cell counts above 200 cells/mm(3) (unmatched controls). Iron parameters including hepcidin were compared using samples collected at cohort enrollment, and compared with recently published reference values for serum hepcidin. RESULTS: A total of 127 HIV-infected patients were included, 42 cases together with 42 matched controls and 43 unmatched controls. Patients with advanced HIV infection had elevated serum hepcidin and ferritin levels. Hepcidin levels correlated inversely with CD4 cells and hemoglobin. Cases had significantly higher hepcidin and ferritin concentrations at cohort enrollment compared to matched controls, but these differences were fully accounted for by the cases who started TB treatment between day 31 and 60 after enrollment. Hepcidin levels were not different in those with or without hepatitis C infection. CONCLUSION: Iron metabolism is distorted in advanced HIV infection with CD4 cell counts correlating inversely with serum hepcidin levels. High serum hepcidin levels and hyperferritinemia were found in patients starting TB treatment shortly after cohort enrollment, suggesting that these parameters have a predictive value for development of manifest TB in HIV-infected patients.
机译:背景:铁稳态的畸变可能有助于人类免疫缺陷病毒(HIV)感染和结核病(TB)的发病。我们研究了中枢铁调节激素hepcidin与HIV严重程度的关系以及hepcidin与铁稳态的其他标志物与结核病发展之间的关系。方法:从印度尼西亚万隆的一个HIV感染对象前瞻性队列中选择三组患者。第一组包括艾滋病病毒感染的患者,这些患者在队列纳入后超过30天开始进行结核病治疗(病例)。第二组由HIV感染的患者组成,这些患者的年龄,性别和CD4细胞计数与病例组相匹配(对照)。第三组包括HIV感染的CD4细胞计数高于200细胞/ mm(3)的患者(无配对对照)。使用队列研究中收集的样本比较了铁参数(包括铁调素),并与最近公布的血清铁调素参考值进行了比较。结果:共纳入127例HIV感染患者,其中42例与42例匹配的对照和43例未匹配的对照一起。晚期HIV感染患者的血清铁调素和铁蛋白水平升高。铁调素水平与CD4细胞和血红蛋白成反比。与匹配的对照组相比,入组患者中铁调素和铁蛋白的浓度显着更高,但这些差异完全由入组后第31天至第60天开始结核病治疗的患者解释。在有或没有丙型肝炎感染者中,铁调素水平没有差异。结论:晚期HIV感染中铁代谢被扭曲,CD4细胞计数与血清铁调素水平成反比。在队列纳入后不久开始结核病治疗的患者中发现高血清铁调素水平和高铁蛋白血症,这表明这些参数对于HIV感染患者明显的结核病发展具有预测价值。

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