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24-Hour profile of serum sclerostin and its association with bone biomarkers in men.

Authors

Swanson C; Shea SA; Wolfe P; Markwardt S; Cain SW; Munch M; Czeisler CA; Orwoll ES; Buxton OM

Source

Osteoporos Int 2017 Nov; 28(11):3205-3213

Link

https://doi.org/10.1007/s00198-017-4162-5

NIOSHTIC No.

20052684

Abstract

Summary: The osteocyte's role in orchestrating diurnal variations in bone turnover markers (BTMs) is unclear. We identified no rhythm in serum sclerostin (osteocyte protein). These results suggest that serum sclerostin can be measured at any time of day and the osteocyte does not direct the rhythmicity of other BTMs in men. Introduction: The osteocyte exerts important effects on bone remodeling, but its rhythmicity and effect on the rhythms of other bone cells are not fully characterized. The purpose of this study was to determine if serum sclerostin displays rhythmicity over a 24-h interval, similar to that of other bone biomarkers. Methods: Serum sclerostin, FGF-23, CTX, and P1NP were measured every 2 h over a 24-h interval in ten healthy men aged 20-65 years. Maximum likelihood estimates of the parameters in a repeated measures model were used to determine if these biomarkers displayed a diurnal, sinusoidal rhythm. Results: No discernible 24-h rhythm was identified for sclerostin (p = 0.99) or P1NP (p = 0.65). CTX rhythmicity was confirmed (p < 0.001), peaking at 05:30 (range 01:30- 07:30). FGF-23 levels were also rhythmic (p < 0.001), but time of peak was variable (range 02:30-11:30). The only significant association identified between these four bone biomarkers was for CTX and P1NP mean 24-h metabolite levels (r = 0.65, p = 0.04). Conclusions: Sclerostin levels do not appear to be rhythmic in men. This suggests that in contrast to CTX, serum sclerostin could be measured at any time of day. The 24-h profiles of FGF-23 suggest that a component of osteocyte function is rhythmic, but its timing is variable. Our results do not support the hypothesis that osteocytes direct the rhythmicity of other bone turnover markers (CTX), at least not via a sclerostinmediated mechanism.

Keywords

Bone structure; Biomarkers; Humans; Men; Proteins; Cell biology; Age groups; Models; Metabolites; Circadian rhythms; TWH; Total Worker Health; Author Keywords: Bone remodeling; Circadian rhythm; Diurnal rhythm; Osteocyte; Sclerostin; Bone turnover

Contact

Christine Swanson, Division of Endocrinology, University of Colorado, 12801 E. 17th Ave. Mail Stop 8106, Aurora, CO 80045

CODEN

OSINEP

Publication Date

20171101

Document Type

Journal Article

Email Address

Christine.Swanson@UCDenver.edu

Funding Type

Cooperative Agreement

Fiscal Year

2018

NTIS Accession No.

NTIS Price

Identifying No.

Cooperative-Agreement-Number-U19-OH-010154

ISSN

0937-941X

Priority Area

Services; Transportation, Warehousing and Utilities

Source Name

Osteoporosis international

State

OR; CO; MA; PA

Performing Organization

Oregon Health & Science University, Portland, Oregon

Page 18 of 59

Page last reviewed: December 9, 2020

Content source: National Institute for Occupational Safety and Health Education and Information Division