Osteoporosis Treatments Affect Bone Matrix Maturation in a Rat Model of Induced Cortical Remodeling

Ryan D Ross; Kyle Anderson; Reid Davison; Bilal M El‐Masri; Christina M Andreasen; Thomas L Andersen; Dale R Sumner

doi:10.1002/jbm4.10344

JBMR Plus (Apr 2020)

Osteoporosis Treatments Affect Bone Matrix Maturation in a Rat Model of Induced Cortical Remodeling

Ryan D Ross,
Kyle Anderson,
Reid Davison,
Bilal M El‐Masri,
Christina M Andreasen,
Thomas L Andersen,
Dale R Sumner

Affiliations

Ryan D Ross: Department of Cell & Molecular Medicine Rush University Medical Center Chicago IL USA
Kyle Anderson: Department of Cell & Molecular Medicine Rush University Medical Center Chicago IL USA
Reid Davison: Department of Cell & Molecular Medicine Rush University Medical Center Chicago IL USA
Bilal M El‐Masri: Clinical Cell Biology, Research Unit of Pathology, Department of Clinical Research University of Southern Denmark, and Department of Pathology, Odense University Hospital Odense Denmark
Christina M Andreasen: Clinical Cell Biology, Research Unit of Pathology, Department of Clinical Research University of Southern Denmark, and Department of Pathology, Odense University Hospital Odense Denmark
Thomas L Andersen: Clinical Cell Biology, Research Unit of Pathology, Department of Clinical Research University of Southern Denmark, and Department of Pathology, Odense University Hospital Odense Denmark
Dale R Sumner: Department of Cell & Molecular Medicine Rush University Medical Center Chicago IL USA

DOI: https://doi.org/10.1002/jbm4.10344
Journal volume & issue: Vol. 4, no. 4
pp. n/a – n/a

Abstract

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ABSTRACT To test how osteoporosis drugs affect bone matrix maturation during cortical bone remodeling, 72 pregnant rats were switched from a 0.4% to a 0.01% calcium diet at parturition for a 23‐day lactation period. At weaning, eight dams were sacrificed to establish baseline values, while the remaining dams were returned to 0.4% calcium and treated with vehicle (saline), sodium fluoride (NaF), zoledronic acid (ZA), or sclerostin antibody (Scl‐Ab) for either 7 or 28 days (eight animals per group per time point). Femora were examined by μCT, dynamic histomorphometry, Fourier transform infrared imaging, and three‐point bending of notched specimens. Cortical porosity decreased in all groups from baseline to day 28. Intracortical mineralizing surface (MS/BS) and mineral apposition rate (MAR), as well as the mineral‐to‐matrix ratio were unaffected by treatment, but intracortical crystallinity was increased in the ZA group at day 10 compared with vehicle. Cortical area increased in all groups over 28 days mainly because of an addition of bone at the endocortical surface. Endocortical MS/BS did not vary among the groups, but endocortical MAR was suppressed in the NaF group at day 2 and elevated in the Scl‐Ab group at day 4 compared with vehicle. Endocortical mineral‐to‐matrix ratio was increased at days 5 and 10 following NaF treatment and endocortical crystallinity was increased at day 5 following ZA treatment compared with vehicle. Fracture toughness did not differ among the groups. Thus, the treatments affected matrix maturation more strongly at the endocortical then intracortical envelope. In this model of induced remodeling, the bone formation phase is synchronized at multiple sites, facilitating study of the effects of drugs or other bone‐targeting agents on matrix maturation independent of their effects on the initiation of remodeling. © 2020 The Authors. JBMR Plus published by Wiley Periodicals, Inc. on behalf of American Society for Bone and Mineral Research.

Published in JBMR Plus

ISSN: 2473-4039 (Online)
Publisher: Oxford University Press
Country of publisher: United Kingdom
LCC subjects: Medicine: Surgery: Orthopedic surgery; Medicine: Internal medicine: Specialties of internal medicine: Diseases of the musculoskeletal system
Website: https://academic.oup.com/jbmrplus

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