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Testosterone Suppresses Hepcidin in Men: A Potential Mechanism for Testosterone-Induced Erythrocytosis

机译:睾丸激素抑制男性中的铁调素:睾丸激素诱导的红细胞增多的潜在机制

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Context: The mechanisms by which testosterone increases hemoglobin and hematocrit are unknown.Objective: The aim was to test the hypothesis that testosterone-induced increase in hematocrit is associated with suppression of the iron regulatory peptide hepcidin.Participants: Healthy younger men (ages 19–35 yr; n = 53) and older men (ages 59–75 yr; n = 56) were studied.Methods: Weekly doses of testosterone enanthate (25, 50, 125, 300, and 600 mg) were administered over 20 wk, whereas endogenous testosterone was suppressed by monthly GnRH agonist administration. Blood and serum parameters from each individual were measured at wk 0, 1, 2, 4, 8, and 20. Longitudinal analyses were performed to examine the relationship between hepcidin, hemoglobin, hematocrit, and testosterone while controlling for potential confounders.Results: High levels of testosterone markedly suppressed serum hepcidin within 1 wk. Hepcidin suppression in response to testosterone administration was dose-dependent in older men and more pronounced than in young men, and this corresponded to a greater rise in hemoglobin in older men. Serum hepcidin levels at 4 and 8 wk were predictive of change in hematocrit from baseline to peak levels.Conclusion: Testosterone administration is associated with suppression of serum hepcidin. Greater increases in hematocrit in older men during testosterone therapy are related to greater suppression of hepcidin.
机译:背景:睾丸激素增加血红蛋白和血细胞比容的机制尚不清楚。目的:目的是检验以下假设:睾丸激素诱导的血细胞比容增加与铁调节肽铁调素的抑制有关。研究对象:健康的年轻男性(19岁至35岁; n = 53)和年龄较大的男性(59-75岁; n = 56)进行了研究。方法:每周服用20周以上的睾丸酮庚酸酯(25、50、125、300和600 mg),而每月施用GnRH激动剂可抑制内源性睾丸激素。在控制潜在的混杂因素的同时,分别在第0、1、2、4、8和20周分别测量了每个人的血液和血清参数。进行了纵向分析,以检查铁调素,血红蛋白,血细胞比容和睾丸激素之间的关系。 1周内睾丸激素水平明显抑制血清铁调素。在老年男性中,响应睾丸激素的铁调素抑制作用是剂量依赖性的,并且比年轻男性更为明显,这对应于老年男性中血红蛋白的升高更大。血清铁调素水平在第4周和第8周可预测血细胞比容从基线到峰值的变化。结论:睾丸激素的施用与血清铁调素的抑制有关。男性睾丸激素治疗期间血细胞比容的更大增加与铁调素的更大抑制有关。

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