Direct modulation of hepatocyte hepcidin signaling by iron

BACKGROUND Liver-secreted hepcidin is the systemic master switch of iron homeostasis and decreased levels of hepcidin are considered to cause iron overload not only in hereditary hemochromatosis but also in hemolytic anemia and chronic liver diseases.The regulation of hepcidin is complex and its response to iron is still not completely understood.AIM To study the direct effect of iron on various established hepcidin signaling pathways in hepatoma cells or primary hepatocytes.METHODS Hepcidin mRNA expression was studied by quantitative real-time(qRT)-PCR in the presence of various forms of iron including ferric ammonium citrate(FAC)in hepatoma cells(Huh7),murine primary hepatocytes and an established co-culture model of phorbol myristate acetate-differentiated THP-1 monocytes and Huh7 cells.To analyze hepcidin signaling,the response to bone morphogenetic protein 6(BMP6),interleukin(IL)-6,IL-1β,hypoxia and lipopolysaccharide(LPS)were studied.Hepcidin and small mothers against decapentaplegic 6(SMAD6)mRNA levels were assessed by qRT-PCR and the expression of phosphorylated signal transducer and activator of transcription 3(phospho-STAT3),STAT3,phospho-SMAD1/5/8 and SMAD1 proteins were analyzed by western blot.RESULTS All iron III forms including FAC efficiently blocked hepcidin mRNA expression at non-toxic dosages in Huh7 cells or primary hepatocytes in a time and dosedependent manner(P<0.001;P<0.05).Hepcidin blockage could be efficiently blunted by iron chelators salicylaldehyde isonicotinoyl hydrazone(SIH)and Desferal(P<0.001).FAC also inhibited BMP6,hypoxia,IL-1βand IL-6-mediated hepcidin induction(P<0.001;P<0.001;P<0.05;P<0.001),and FAC also inhibited LPS-mediated hepatic hepcidin induction in co-culture model(P<0.001).Moreover,FAC reduced SMAD6 mRNA and p-SMAD1/5/8 protein expression at basal or upon stimulation by BMP6(P<0.05;P<0.01),and FAC also reduced SMAD6 and p-SMAD1/5/8 expression under hypoxia(P<0.01;P<0.05).However,FAC has no significant effect on p-STAT3 protein expression at basal or upon stimulation by various stimuli.Notably,in the presence of the BMP/SMAD signaling pathway inhibitor LDN193189 Hydrochloride(LDN),FAC was unable to further decrease hepcidin,SMAD6 and p-SMAD1/5/8 expression compared with LDN alone.CONCLUSION Iron directly blocks hepatocellular hepcidin signaling through the BMP/SMAD pathway but independent of STAT3.This mechanism may contribute to continued iron overload in many pathophysiological conditions ultimately causing a vicious cycle of continued hepcidin suppression.

不同运动方式对大鼠血清与肝脏中hepcidin水平及相关调节因素的影响

目的:比较耐力运动及力竭运动对大鼠血液及肝脏中铁调素(hepcidin)表达的影响,并测定分析与之相关的铁代谢指标、低氧应答因子、炎性因子、抗菌肽活性相关指标的变化趋势。方法:雌性SD大鼠30只,随机分为对照组(n=10)、耐力运动组(n=10)、力竭运动组(n=10),对照组不运动,耐力运动组和力竭运动组分别采用为期4周的中等运动强度跑台训练和力竭运动强度跑台训练对大鼠进行干预,而后分别采集血样,进行血常规指标及血清中铁转运因子、低氧应答因子、炎性因子及抗菌肽活性相关指标测定;取肝脏标本,固定、包埋、切片后,利用免疫组织化学染色分别测定不同组别动物肝脏中hepcidin、低氧诱导因子(HIF-1α)、核转录因子kappa b(NF-κB)含量。结果:与对照组相比,4周耐力性运动后大鼠血清中hepcidin水平降低(P<0.05),促红细胞生成素(EPO)浓度升高(P<0.05),白细胞介素6(IL-6)浓度下降(P<0.01)。与对照组相比,4周力竭性运动后大鼠血清及肝脏中hepcidin水平升高(P<0.01),EPO浓度降低(P<0.01),同时伴有血清及肝脏中HIF-1α表达增加(P<0.01),血清转铁蛋白(TF)、可溶性转铁蛋白受体(s TFR)水平降低(P<0.01),血清中白细胞介素1(IL-1)、IL-6、肿瘤坏死因子α(TNF-α)、C反应蛋白(CRP)水平显著升高(P<0.01,P<0.001,P<0.001,P<0.001);同时血清中与hepcidin抗菌肽活性相关的toll样受体4(TLR4)、NF-κB水平均显著升高(P<0.001)。结论:4周耐力性运动可下调大鼠血清中hepcidin水平;而4周力竭性运动可使大鼠血清及肝脏中hepcidin水平显著上调,提示不同运动方式对hepcidin的影响存在明显差异。

大强度运动后低氧对大鼠炎症反应和十二指肠铁吸收蛋白的影响

目的:研究低氧对大鼠炎症反应和肠铁吸收相关蛋白的影响,阐明低氧影响机体铁状态的调节机制。方法:24只雄性Wistar大鼠随机分为安静对照组(C组)、大强度运动组(E组)和运动后低氧恢复组(HE组)。E组和HE组进行递增负荷跑台运动,坡度0,速度30 m/min,6 d/周,前2周1次/天,后2周2次/天,共4周。训练第1次为1 min,每次递增2 min。HE组每天运动后在13.6%O2的低氧舱中休息,8 h/d。检测各组血清铁,ELISA法检测血清铁调素(hepcidin)和白介素6(IL-6),Western Blot法检测十二指肠铁转运蛋白:血红素转运体1(Heme transport protein1,HCP1)、二价金属离子转运蛋白1(divalent metal transporter 1,DMT1)和膜铁转运蛋白1(Ferroportin 1,FPN1)表达。结果:(1)HE组血清铁和Hb显著高于C组和E组(P<0.01,P<0.05),血清hepcidin、IL-6、白细胞数显著低于E组(P<0.05);而E组血清铁和Hb显著低于C组(P<0.05,P<0.01)。(2)HE组HCP1、DMT1、FPN1均显着高于C组和E组(P<0.01,P<0.05)。结论:适度低氧降低运动机体炎症反应,减少肝分泌hepcidin,促进肠铁吸收,改善机体铁状态,预防运动性铁缺乏。