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年龄和性别对血清骨膜蛋白的影响:与皮质测量、骨转换及激素的关系

Effect of age and gender on serum periostin: Relationship to cortical measures, bone turnover and hormones.

作者信息

Walsh Jennifer S, Gossiel Fatma, Scott Jessica R, Paggiosi Margaret A, Eastell Richard

机构信息

Mellanby Centre for Bone Research, University of Sheffield, UK.

Mellanby Centre for Bone Research, University of Sheffield, UK.

出版信息

Bone. 2017 Jun;99:8-13. doi: 10.1016/j.bone.2017.03.041. Epub 2017 Mar 16.

DOI:10.1016/j.bone.2017.03.041
PMID:28323143
Abstract

Periostin is an extracellular matrix protein, and in bone is expressed most highly in the periosteum. It increases bone formation through osteoblast differentiation, cell adhesion, Wnt signalling and collagen cross-linking. We hypothesised that serum periostin would be high at times of life when cortical modeling is active, in early adulthood and in older age, and that it would correlate with cortical bone measures, bone turnover and hormones that regulate cortical modeling. We conducted a cross-sectional observational study of 166 healthy men and women at three skeletal stages; the end of longitudinal growth (16-18years), peak bone mass (30-32years) and older age (over 70years). We measured serum periostin with a new ELISA optimised for human serum and plasma which recognises all known splice variants (Biomedica). We measured the distal radius and distal tibia with HR-pQCT, and measured serum PINP, CTX, sclerostin, PTH, IGF-1, estradiol and testosterone. Periostin was higher at age 16-18 than age 30-32 (1253 vs 842pmol/l, p<0.001), but not different between age 30-32 and over age 70. Periostin was inversely correlated with tibia cortical thickness and density (R -0.229, -0.233, both p=0.003). It was positively correlated with PINP (R 0.529, p<0.001), CTX (R 0.427, p<0.001) and IGF-1 (R 0.440, p<0.001). When assessed within each age group these correlations were only significant at age 16-18, except for PINP which was also significant over age 70. We conclude that periostin may have a role in IGF-1 driven cortical modeling and consolidation in young adults, but it may not be an important mediator in older adults.

摘要

骨膜蛋白是一种细胞外基质蛋白,在骨骼中,它在骨膜中的表达最为丰富。它通过成骨细胞分化、细胞黏附、Wnt信号传导和胶原蛋白交联来促进骨形成。我们推测,在皮质骨塑形活跃的生命时期,即成年早期和老年期,血清骨膜蛋白水平会升高,并且它会与皮质骨测量指标、骨转换以及调节皮质骨塑形的激素相关。我们对166名处于三个骨骼阶段的健康男性和女性进行了一项横断面观察研究;纵向生长结束时(16 - 18岁)、骨量峰值时(30 - 32岁)以及老年期(70岁以上)。我们使用一种针对人血清和血浆优化的新型酶联免疫吸附测定法(ELISA)测量血清骨膜蛋白,该方法可识别所有已知的剪接变体(Biomedica公司)。我们使用高分辨率外周定量CT(HR - pQCT)测量桡骨远端和胫骨远端,并测量血清I型前胶原氨基端前肽(PINP)、I型胶原交联C端肽(CTX)、硬化蛋白、甲状旁腺激素(PTH)、胰岛素样生长因子 - 1(IGF - 1)、雌二醇和睾酮。16 - 18岁时的骨膜蛋白水平高于30 - 32岁时(1253对842pmol/l,p<0.001),但30 - 32岁和70岁以上者之间无差异。骨膜蛋白与胫骨皮质厚度和密度呈负相关(R分别为 - 0.229、 - 0.233,p均为0.003)。它与PINP(R 0.529,p<0.001)、CTX(R 0.427,p<0.001)和IGF - 1(R 0.440,p<0.001)呈正相关。在每个年龄组内进行评估时,这些相关性仅在16 - 18岁时显著,PINP除外,其在70岁以上时也显著。我们得出结论,骨膜蛋白可能在成年早期由IGF - 1驱动的皮质骨塑形和巩固过程中起作用,但在老年人中可能不是重要的调节因子。

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