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铁调素对人成骨细胞(hFOB1.19)内钙离子转运的影响 被引量:13

Effect of Hepcidin out of Osteoblast on Calcium Transportation
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摘要 目的研究铁调素对人成骨细胞(hFOB 1.19)内Ca2+转运的影响。方法将成骨细胞34℃下培养3~4 d至细胞密度为90%,用胰蛋白酶消化后分种于12孔培养板。空白组加双蒸水;实验组加不同浓度铁调素(双蒸水配制),包括H1组(终浓度为10 nmol/L)和H2组(终浓度为50 nmol/L)。干预24 h后用激光共聚焦扫描显微镜(CLSM)检测。结果成骨细胞内钙离子荧光强度空白组为56.38±36.47,H1组为68.01±32.90;H2组为154.06±55.62,3组间的差异有统计学意义(P<0.05)。结论铁调素可促进成骨细胞内Ca2+浓度增加。 0bjective To study the effect of hepcidin concentrations change out of hFOB 1.19 cells on calcium transportation.Methods The hFOB 1.19 was cultured at 34℃ for 3~4 d,being digested with trypsin,then placed in the culture board.D2H2O was added in the control group and hepcidin of different concentration in the experiment group:H1 group(the final concentration was 10 nmol/L) and H2 group(the final concentration is 50 nmol/L).Confocal laser scanning microscope(CLSM) was used in this study 24 hours later.Results...
作者 张鹏 徐又佳 赵东阳 王冰 马勇 钱忠明 柯亚
机构地区 苏州大学附属第二医院骨科 香港理工大学 香港中文大学
出处 《苏州大学学报(医学版)》 CAS 北大核心 2008年第1期14-15,37+2,共4页 Suzhou University Journal of Medical Science
基金 江苏省高校自然科学基金资助课题(05KJB320125) 江苏省六大高峰人才项目(07-B-032) 江苏省医学重点人才项目(RC2007100)
关键词 铁调素 钙离子 铁离子 人成骨细胞(hFOB1.19) 激光共聚焦扫描显微镜 hepcidin Ca2+ Fe3+ hFOB1.19 confocal laser scanning microscope(CLSM)
分类号 R68 [医药卫生—骨科学]
  • 相关文献

参考文献6

  • 1马勇,徐又佳,王爱东,俞晨,王冰,张鹏,张振东.大鼠骨质疏松模型中肝脏Hepcidin基因表达的初步研究[J].苏州大学学报(医学版),2006,26(3):367-369. 被引量:12
  • 2徐又佳,钱忠明,俞晨.铁调素(Hepcidin)在骨质矿化中的作用[J].中国骨质疏松杂志,2005,11(4):541-543. 被引量:16
  • 3[3]Park CH,Valore EV,Waling AJ,et al.Hepcidin,a urinary antimicrobial peptide synthesized in the liver[J].Journal of Biological Chemistry,2001,276(11):7806-7810.
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  • 5[5]Maurer J,Harris MM,Stanford VA,et al.Dietary iron positively influences bone mineral density in postmenopausal women on hormone replacement therapy[J].Journal of Nutrition,2005,135(4):863-869.
  • 6[6]Schnitzler C.M,Schnaid E,MacPhail A.P,et al.Ascorbie acid deficiency,iron overload and alcohol abuse underlie the severe osteoporosis in black african patients with hip fractures-a bone histomorphometric study[J].Calcif Tissue Int.,2005,76(2):79-89.

二级参考文献15

  • 1钱忠明,蒲咏梅,邓柏礼.网织红细胞铁摄取机制的研究进展[J].生物化学与生物物理进展,1997,24(1):8-13. 被引量:12
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共引文献22

同被引文献157

  • 1郭晓强.海帕西啶与铁代谢[J].基础医学与临床,2005,25(9):794-797. 被引量:6
  • 2徐又佳,钱忠明,俞晨.铁调素(Hepcidin)在骨质矿化中的作用[J].中国骨质疏松杂志,2005,11(4):541-543. 被引量:16
  • 3马勇,徐又佳,王爱东,俞晨,王冰,张鹏,张振东.大鼠骨质疏松模型中肝脏Hepcidin基因表达的初步研究[J].苏州大学学报(医学版),2006,26(3):367-369. 被引量:12
  • 4Parelman M, Stoeeker B, Baker A, et al. Iron restriction negatively affects bone in female rats and mineralization of hFOB osteoblast cells. Experim Biol Med, 2006,231:378-386.
  • 5Mauler J,Harris MM, Stanford VA, et al. Dietary iron positively influences bone mineral density in postmenopausal women on hormone replacement therapy. J Nutr, 2005,135 (4) :863-869.
  • 6Simonet WS, Laeey DL, Dunstan CR, et al. Osteopmtegerin: a novel secreted protein involved in the regulation of bone density.Cell, 1997,89:309-319.
  • 7Schoppet M, Prelssner KT, Hofbauer LC. RANK ligand and osteoprotegerin: paracrine regulators of bone metabolism and vascular function. Arterioselcr Thromb Vasc Biol, 2002,22:549- 553.
  • 8Swaminathan R. Biochemical markers of bone turnover. Clin Chim Acta, 2001,313:95-105.
  • 9Tomas Ganz, Elizabeta Nemeth. Regulation of iron acquisition and iron distribution in mammals. Biochimica et Biophysiea Acta, 2006, 1763:690-699.
  • 10Schnitzler CM, Schnaid E, MacPhail AP, et al. Ascorbic acid deficiency, iron overload and alcohol abuse underlie the severe osteoporosis in black African patients with hip fractures-a bone histomorphometric study. Calcif Tissue Int,2005,76(2):79-89.

引证文献13

二级引证文献57

苏州大学学报(医学版)
2008年 第1期

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