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低剂量重组促红细胞生成素治疗的人类受试者全身和肌肉铁代谢的改变。

Alterations of systemic and muscle iron metabolism in human subjects treated with low-dose recombinant erythropoietin.

作者信息

Robach Paul, Recalcati Stefania, Girelli Domenico, Gelfi Cecilia, Aachmann-Andersen Niels J, Thomsen Jonas J, Norgaard Anne M, Alberghini Alessandra, Campostrini Natascia, Castagna Annalisa, Viganò Agnese, Santambrogio Paolo, Kempf Tibor, Wollert Kai C, Moutereau Stéphane, Lundby Carsten, Cairo Gaetano

机构信息

Département Médical, Ecole Nationale de Ski et d'Alpinisme, Chamonix, France.

出版信息

Blood. 2009 Jun 25;113(26):6707-15. doi: 10.1182/blood-2008-09-178095. Epub 2009 Mar 4.

Abstract

The high iron demand associated with enhanced erythropoiesis during high-altitude hypoxia leads to skeletal muscle iron mobilization and decrease in myoglobin protein levels. To investigate the effect of enhanced erythropoiesis on systemic and muscle iron metabolism under nonhypoxic conditions, 8 healthy volunteers were treated with recombinant erythropoietin (rhEpo) for 1 month. As expected, the treatment efficiently increased erythropoiesis and stimulated bone marrow iron use. It was also associated with a prompt and considerable decrease in urinary hepcidin and a slight transient increase in GDF-15. The increased iron use and reduced hepcidin levels suggested increased iron mobilization, but the treatment was associated with increased muscle iron and L ferritin levels. The muscle expression of transferrin receptor and ferroportin was up-regulated by rhEpo administration, whereas no appreciable change in myoglobin levels was observed, which suggests unaltered muscle oxygen homeostasis. In conclusion, under rhEpo stimulation, the changes in the expression of muscle iron proteins indicate the occurrence of skeletal muscle iron accumulation despite the remarkable hepcidin suppression that may be mediated by several factors, such as rhEpo or decreased transferrin saturation or both.

摘要

高海拔缺氧期间红细胞生成增强所伴随的高铁需求会导致骨骼肌铁动员以及肌红蛋白水平降低。为了研究在非缺氧条件下红细胞生成增强对全身和肌肉铁代谢的影响,8名健康志愿者接受了重组促红细胞生成素(rhEpo)治疗1个月。正如预期的那样,该治疗有效地增加了红细胞生成并刺激了骨髓铁利用。它还与尿铁调素迅速且显著降低以及生长分化因子15(GDF - 15)轻微短暂升高有关。铁利用增加和铁调素水平降低表明铁动员增加,但该治疗与肌肉铁和L - 铁蛋白水平升高有关。rhEpo给药上调了转铁蛋白受体和铁转运蛋白在肌肉中的表达,而肌红蛋白水平未观察到明显变化,这表明肌肉氧稳态未改变。总之,在rhEpo刺激下,肌肉铁蛋白表达的变化表明尽管铁调素受到显著抑制,而这种抑制可能由多种因素介导,如rhEpo或转铁蛋白饱和度降低或两者共同作用,但骨骼肌仍出现了铁蓄积。

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