基础医学与临床 ›› 2009, Vol. 29 ›› Issue (5): 504-509.

• 研究论文 • 上一篇    下一篇

FGF23、MEPE和sFRP4在肿瘤性骨软化症发病机制中的作用

姜艳 夏维波 孟迅吾 邢小平 李梅 王鸥 胡莹莹 刘怀成 周学瀛   

  1. 北京协和医院 北京协和医院内分泌科 北京协和医院内分泌科 北京协和医院内分泌科 中国医学科学院北京协和医学院北京协和医院内分泌科 北京协和医院
  • 收稿日期:2008-12-26 修回日期:2009-02-19 出版日期:2009-05-25 发布日期:2009-05-25

The role of fibroblast growth factor 23, matrix extracellular phosphoglycoprotein and secreted frizzled related protein 4 in pathogenesis of tumor induced osteomalacia

Yan JIANG, Wei-bo XIA, Xun-wu MENG, Xiao-ping XING, Mei LI, Ou WANG, Ying-ying HU, Huai-cheng LIU, Xue-ying ZHOU   

  1. PUMC Hospital,CAMS & PUMC PUMC Hospital,CAMS & PUMC Department of Endocrinology, Key laboratory of Ministry of Health, PUMC Hospital, CAMS & PUMC Department of Endocrinology, key Lab of the Health Ministry, Peking Union Medical College Hospital,Peking Union Medical College, Chinese Academy of Medical Sciences,
  • Received:2008-12-26 Revised:2009-02-19 Online:2009-05-25 Published:2009-05-25

摘要: 目的 探讨成纤维细胞生长因子-23(FGF-23)、细胞外基质磷酸糖蛋白(MEPE)和分泌型卷曲相关蛋白(sFRP4)在肿瘤性骨软化症(TIO)发病机制中的作用。方法 TIO肿瘤8例(T1-T8),其他间叶肿瘤5例(C1-C5),低血磷骨软化症病人行股骨手术,病理为凝血坏死组织1例(P1),正常人骨骼、肌肉组织各2例(B1、B2、M1和M2)。RT-PCR检测组织中FGF23、MEPE、sFRP4 mRNA的表达,Western blot检测TIO肿瘤FGF23蛋白的表达。TIO 4例(T1、T3、T4和T7)及P1在手术前后分别取血测定血清磷和FGF23(ELISA)水平。结果 TIO肿瘤有数量不等的FGF23和MEPE的mRNA表达,部分肿瘤表达sFRP4的mRNA。7/8例TIO肿瘤有不同强度FGF23蛋白表达。TIO术前血FGF23升高,术后2~24h降至正常;血磷3~10d缓慢升至正常, P1病人术后血FGF23无变化,血磷未上升。FGF23与MEPE mRNA正相关(r=0.884,P<0.05),FGF23 mRNA与蛋白表达之间成正相关关系(r=0.921,P<0.05)。结论 FGF23是TIO发病的主要原因,MEPE在TIO肿瘤发病中起到一定作用,sFRP4的作用尚不明确。

关键词: 肿瘤性骨软化症, 成纤维细胞生长因子23, 细胞外基质磷酸糖蛋白, 分泌型卷曲相关蛋白4

Abstract: Objective To evaluate the role of Fibroblast growth factor 23 (FGF-23), matrix extracellular phosphoglycoprotein (MEPE) and secreted Frizzled related protein 4 (sFRP4) in pathogenesis of Tumor induced osteomalacia (TIO). Methods The mRNA expressions of FGF23, MEPE and sFRP4 were detected in 8 TIO tumors (T1-T8), 5 other mesenchymal tumors(C1-C5), 2 normal bone tissues(B1-B2), 2 normal muscle tissues(M1-M2), blood clotting and necrostic tissue of bone in a patient of hypophospatemic osteomalacia but not TIO (P1) using RT-PCR. The FGF23 protein expressions were analyzed in 8 TIO tumors using Western blot. Serum FGF23 (ELISA) and phosphate were measured before and after operation in 4 TIO (T1、3、4、7) and P1 patients. Results The mRNA of FGF23 and MEPE were expressed in TIO tumors abundantly. Some TIO tumors expressed sRP4 mRNA. 7/8 TIO tumors expressed various FGF23 protein in Western blot. Serum FGF23 in TIO patients were elevated, and went down after tumor resections in 2~24 hrs. The increase of serum phosphate was slower than FGF23 degression (in 3~10 days). Serum FGF23 was stably high in P1 patient without serum phosphate elevation. The expressions of FGF23 and MEPE mRNA were related (r=0.884,P<0.05). There was a positive relationship between FGF23 mRNA and protein expression (r=0.921,P<0.05). Conclusions FGF23 plays an important role in pathogenesis of TIO. MEPE may be involved in pathogenesis of TIO. The role of sFRP4 in pathogenesis of TIO is still need to be explored.

Key words: tumor induced osteomalacia, fibroblast growth factor 23, matrix extracellular phosphoglycoprotein, secreted frizzled related protein 4