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首页> 外文期刊>European Journal of Applied Physiology >Early effects of erythropoietin on serum hepcidin and serum iron bioavailability in healthy volunteers
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Early effects of erythropoietin on serum hepcidin and serum iron bioavailability in healthy volunteers

机译:促红细胞生成素对健康志愿者血清铁调素和血清铁生物利用度的早期影响

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Hepcidin regulates plasma iron bioavailability and subsequently iron availability for erythropoiesis. rHuEPO has been reported to decrease hepcidin expression in case of repeated subcutaneous injections. Thus, hepcidin level measurement could be a candidate marker for detection of rHuEPO abuse. However, when used for doping, rHuEPO can be injected intravenously and the scheme of injection is unknown. Our aim was to evaluate the early effects of a single intravenous rHuEPO injection on serum hepcidin levels. Fourteen male healthy volunteers received one intravenous injection of 50 U/Kg of rHuEPO during a placebo-controlled, randomized, double-blind, cross-over study. Serum hepcidin, quantified by a competitive ELISA method and iron parameters was then evaluated for 24 h. Serum levels of hepcidin were significantly increased 4 h after rHuEPO injection when compared with placebo injection (78.3 ± 55.5 vs. 57.5 ± 34.6 ng/ml, respectively; +36%, p 0.05), whereas iron and transferrin saturation dramatically decreased 12 h after rHuEPO injection when compared with placebo injection (9.2 ± 3.5 vs. 15.8 ± 4.2 μg/l, respectively; −42%, p 0.05 and 14.8 ± 5.0 vs. 26.3 ± 6.4%, respectively; −44%, p 0.05). In addition, 12 and 24 h after rHuEPO injection serum hepcidin levels were lower compared with placebo injection (41.6 ± 27.4 vs. 56.6 ± 28.1 ng/ml after 12 h; −27%, p 0.05 and 26.0 ± 29.6 vs. 81.2 ± 29.4 ng/ml after 24 h; −68%, p 0.05). Intravenous injection of recombinant EPO induces a precocious and transient increase of serum hepcidin leading to a transient decrease of iron bioavailability. The transitory increase and dynamics of its concentration make difficult the practical use of hepcidin to detect rHuEPO doping.
机译:Hepcidin调节血浆铁的生物利用度,进而调节红细胞生成的铁利用度。据报道,在反复皮下注射的情况下,rHuEPO会降低铁调素的表达。因此,铁调素水平的测量可能是检测rHuEPO滥用的候选标记。然而,当用于掺杂时,rHuEPO可以静脉内注射,并且注射方案是未知的。我们的目的是评估单次静脉内注射rHuEPO对血清铁调素水平的早期影响。在安慰剂对照,随机,双盲,交叉研究中,十四名男性健康志愿者接受了一次静脉注射50 U / Kg rHuEPO。然后通过竞争性ELISA方法定量血清铁调素和铁参数24小时。与安慰剂注射相比,rHuEPO注射后4 h的血清铁调素水平显着增加(分别为78.3±55.5和57.5±34.6 ng / ml; + 36%,p <0.05),而铁和转铁蛋白饱和度显着降低12 h与安慰剂注射相比,rHuEPO注射后(分别为9.2±3.5 vs. 15.8±4.2μg/ l; -42%,p <0.05和14.8±5.0 vs. 26.3±6.4%; -44%,p <0.05 )。此外,rHuEPO注射后12和24 h,血清铁调素水平低于安慰剂注射(12 h后为41.6±27.4 vs. 56.6±28.1 ng / ml; −27%,p <0.05和26.0±29.6 vs. 81.2± 24小时后为29.4 ng / ml; -68%,p <0.05)。静脉内注射重组EPO会导致血清铁调素过早和短暂地增加,从而导致铁生物利用度的短暂下降。瞬时增加及其浓度的动态变化使铁调素的实际应用难以检测rHuEPO掺杂。

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