绝经前女性的血清成纤维细胞生长因子23、血清铁与骨密度
Serum fibroblast growth factor 23, serum iron and bone mineral density in premenopausal women.
作者信息
Imel Erik A, Liu Ziyue, McQueen Amie K, Acton Dena, Acton Anthony, Padgett Leah R, Peacock Munro, Econs Michael J
机构信息
Department of Medicine, Indiana University School of Medicine, USA; Department of Pediatrics, Indiana University School of Medicine, USA.
Indiana University School of Public Health, Department of Biostatistics, USA.
出版信息
Bone. 2016 May;86:98-105. doi: 10.1016/j.bone.2016.03.005. Epub 2016 Mar 8.
Fibroblast growth factor 23 (FGF23) circulates as active protein and inactive fragments. Low iron status increases FGF23 gene expression, and iron deficiency is common. We hypothesized that in healthy premenopausal women, serum iron influences C-terminal and intact FGF23 concentrations, and that iron and FGF23 associate with bone mineral density (BMD). Serum iron, iron binding capacity, percent iron saturation, phosphorus, and other biochemistries were measured in stored fasting samples from healthy premenopausal white (n=1898) and black women (n=994), age 20-55years. Serum C-terminal and intact FGF23 were measured in a subset (1631 white and 296 black women). BMD was measured at the lumbar spine and femur neck. Serum phosphorus, calcium, alkaline phosphatase and creatinine were lower in white women than black women (p<0.001). Serum iron (p<0.0001) and intact FGF23 (p<0.01) were higher in white women. C-terminal FGF23 did not differ between races. Phosphorus correlated with intact FGF23 (white women, r=0.120, p<0.0001; black women r=0.163, p<0.01). However, phosphorus correlated with C-terminal FGF23 only in black women (r=0.157, p<0.01). Intact FGF23 did not correlate with iron. C-terminal FGF23 correlated inversely with iron (white women r=-0.134, p<0.0001; black women r=-0.188, p<0.01), having a steeper slope at iron <50mcg/dl than ≥50mcg/dl. Longitudinal changes in iron predicted changes in C-terminal FGF23. Spine BMD correlated with iron negatively (r=-0.076, p<0.01) in white women; femur neck BMD correlated with iron negatively (r=-0.119, p<0.0001) in black women. Both relationships were eliminated in weight-adjusted models. BMD did not correlate with FGF23. Serum iron did not relate to intact FGF23, but was inversely related to C-terminal FGF23. Intact FGF23 correlated with serum phosphorus. In weight-adjusted models, BMD was not related to intact FGF23, C-terminal FGF23 or iron. The influence of iron on FGF23 gene expression is not important in determining bone density in healthy premenopausal women.
成纤维细胞生长因子23(FGF23)以活性蛋白和无活性片段的形式在血液中循环。低铁状态会增加FGF23基因的表达,而缺铁情况很常见。我们假设,在健康的绝经前女性中,血清铁会影响C末端和完整FGF23的浓度,并且铁和FGF23与骨矿物质密度(BMD)相关。我们对年龄在20 - 55岁的健康绝经前白人女性(n = 1898)和黑人女性(n = 994)的空腹储存样本进行了血清铁、铁结合能力、铁饱和度百分比、磷及其他生物化学指标的检测。在一个子集中(1631名白人女性和296名黑人女性)检测了血清C末端和完整FGF23。在腰椎和股骨颈处测量了骨密度。白人女性的血清磷、钙、碱性磷酸酶和肌酐低于黑人女性(p < 0.001)。白人女性的血清铁(p < 0.0001)和完整FGF23(p < 0.01)较高。C末端FGF23在不同种族之间没有差异。磷与完整FGF23相关(白人女性,r = 0.120,p < 0.0001;黑人女性,r = 0.163,p < 0.01)。然而,磷仅在黑人女性中与C末端FGF23相关(r = 0.157,p < 0.01)。完整FGF23与铁不相关。C末端FGF23与铁呈负相关(白人女性,r = -0.134,p < 0.0001;黑人女性,r = -0.188,p < 0.01),在铁<50mcg/dl时的斜率比≥50mcg/dl时更陡。铁的纵向变化可预测C末端FGF23的变化。白人女性的脊柱骨密度与铁呈负相关(r = -0.076,p < 0.01);黑人女性的股骨颈骨密度与铁呈负相关(r = -0.119,p < 0.0001)。在体重调整模型中,这两种关系均消失。骨密度与FGF23不相关。血清铁与完整FGF23无关,但与C末端FGF23呈负相关。完整FGF23与血清磷相关。在体重调整模型中,骨密度与完整FGF23、C末端FGF23或铁均无关。在健康绝经前女性中,铁对FGF23基因表达的影响在决定骨密度方面并不重要。
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