在由LRP5基因突变导致骨量高的个体中，硬化蛋白、Dickkopf-1和分泌型卷曲相关蛋白4的血清水平未发生变化。

Serum levels of sclerostin, Dickkopf-1, and secreted frizzled-related protein-4 are not changed in individuals with high bone mass causing mutations in LRP5.

作者信息

Simpson C A, Foer D, Lee G S, Bihuniak J, Sun B, Sullivan R, Belsky J, Insogna K L

机构信息

Department of Medicine, Section of Endocrinology, Yale School of Medicine, 330 Cedar Street, P.O.Box 208020, New Haven, CT, 06520-8020, USA,

出版信息

Osteoporos Int. 2014 Oct;25(10):2383-8. doi: 10.1007/s00198-014-2767-5. Epub 2014 Jun 14.

DOI:10.1007/s00198-014-2767-5

PMID:24927689

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4659359/

Abstract

SUMMARY

We compared circulating levels of Wnt inhibitors among patients with high bone mass mutations in LRP5, unaffected kindred, and unrelated normal controls. Inhibitors were unchanged in affected and unaffected kindred. We saw no meaningful differences between controls and affected individuals. LRP5 signaling may not influence circulating levels of these inhibitors.

INTRODUCTION

It is thought that gain-of-function mutations in LRP5 result in high bone mass syndromes because these allelic variants confer resistance to the actions of endogenous inhibitors of Wnt signaling. We therefore attempted to determine if circulating levels of Wnt inhibitors are altered in patients with gain-of-function mutations in LRP5.

METHODS

This is a cross-sectional study in a university research center. Serum was collected from consented volunteers known to have either the G171V or N198S gain-of-function mutations in LRP5, kindred members affected with either mutation, unrelated kindred, and unrelated normal age-matched controls. BMD was provided or measured on site.

RESULTS

There were no significant differences found in the serum levels of sclerostin (SOST), Dickkopf-1 (Dkk-1), or secreted frizzled-related protein-4 (SFRP-4) in affected vs. unaffected individuals from different kindreds or when compared to age-matched unrelated normal individuals. Mean serum SOST values in affected and unaffected kindred members and unrelated normal controls were 52.7 ± 6.1, 36.5 ± 9.6, and 54.8 ± 5.4, respectively. For Dkk-1, the values were 25.9 ± 3.4, 25.7 ± 3.0, and 17.3 ± 2.3 and for SFRP-4, 38.1 ± 2.3, 39.8 ± 3.6, and 28.5 ± 1.7. Serum levels of RANKL and osteoprotegerin (OPG) were not different in the three groups.

CONCLUSIONS

Circulating levels of endogenous Wnt inhibitors do not change in patients with gain-of-function mutations in LRP5 including Dkk1, which is suppressed by Wnt signaling. It may be that circulating levels of Wnt inhibitors do not reflect changes in target tissues. It is also possible that other mechanisms besides or in addition to resistance in Wnt inhibitors explains the skeletal effects of these mutations.

摘要

我们比较了LRP5基因存在高骨量突变的患者、未受影响的亲属以及无关正常对照者体内Wnt抑制剂的循环水平。在受影响和未受影响的亲属中，抑制剂水平没有变化。我们发现对照者与受影响个体之间没有显著差异。LRP5信号通路可能不会影响这些抑制剂的循环水平。

引言

人们认为LRP5基因的功能获得性突变会导致高骨量综合征，因为这些等位基因变异赋予了对Wnt信号通路内源性抑制剂作用的抗性。因此，我们试图确定LRP5基因功能获得性突变患者体内Wnt抑制剂的循环水平是否发生改变。

方法

这是一项在大学研究中心进行的横断面研究。从已知携带LRP5基因G171V或N198S功能获得性突变的自愿参与者、受任一突变影响的亲属、无关亲属以及年龄匹配的无关正常对照者中采集血清。现场提供或测量骨密度。

结果

在来自不同亲属的受影响与未受影响个体之间，或者与年龄匹配的无关正常个体相比，硬化蛋白（SOST）、Dickkopf-1（Dkk-1）或分泌型卷曲相关蛋白-4（SFRP-4）的血清水平没有显著差异。受影响和未受影响的亲属成员以及无关正常对照者的血清SOST平均水平分别为52.7±6.1、36.5±9.6和54.8±5.4。Dkk-1的水平分别为25.9±3.4、25.7±3.0和17.3±2.3，SFRP-4的水平分别为38.1±2.3、39.8±3.6和28.5±1.7。三组中核因子κB受体活化因子配体（RANKL）和骨保护素（OPG）的血清水平没有差异。