Cortical porosity is elevated after a single dose of zoledronate in two rodent models of chronic kidney disease

Cortical porosity is elevated after a single dose of zoledronate in two rodent models of chronic kidney disease

Patients with chronic kidney disease (CKD) have high risk of fracture in part due to cortical bone deterioration. The goal of this study was to assess the impact of two different bisphosphonates and dosing regimens on cortical microstructure (porosity, thickness, area) and bone mechanical properties...

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Bibliographic Details
Published in:Bone Reports Vol. 16; p. 101174
Main Authors: Swallow, Elizabeth A., Metzger, Corinne E., Chen, Neal X., Wallace, Joseph M., Tippen, Samantha P., Kohler, Rachel, Moe, Sharon M., Allen, Matthew R.
Format: Journal Article
Language:English
Published: United States Elsevier Inc 01-06-2022
Elsevier
Subjects:
Bisphosphonates
Bone
Chronic kidney disease (CKD)
Cortical porosity
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Cortical porosity
Bone
Bisphosphonates
Chronic kidney disease (CKD)
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Summary:Patients with chronic kidney disease (CKD) have high risk of fracture in part due to cortical bone deterioration. The goal of this study was to assess the impact of two different bisphosphonates and dosing regimens on cortical microstructure (porosity, thickness, area) and bone mechanical properties in animal models of CKD. In experiment 1, Male Cy/+ (CKD) rats were treated with either a single dose or ten fractionated doses of zoledronate at 18 weeks of age. Fractionated animals received 1/10th of single dose given weekly for 10 weeks, with study endpoint at 28 weeks of age. In experiment 2, male C57Bl/6 J mice were given dietary adenine (0.2%) to induce CKD. Bisphosphonate treated groups were given either a single dose of zoledronate or weekly risedronate injections for 4 weeks. Cortical microstructure was assessed via μCT and mechanical parameters evaluated by monotonic bending tests. Exp 1: CKD rats had higher blood urea nitrogen (BUN) and parathyroid hormone (PTH) compared to NL littermate controls. Single dose zoledronate had significantly higher cortical porosity in CKD S.Zol (2.29%) compared to NL control (0.04%) and untreated CKD (0.14%) (p = 0.004). Exp 2: All adenine groups had significantly higher BUN and PTH compared to control mice. Mice treated with single dose zoledronate (Ad + Zol) had the highest porosity (~6%), which was significantly higher compared to either Ad or Ad + Ris (~3%; p < 0.0001) and control mice had the lowest cortical porosity (0.35%). In both experiments, mechanics were minimally affected by any bisphosphonate dosing regimen. A single dose of zoledronate leads to higher cortical porosity compared to more frequent dosing of bisphosphonates (fractionated zoledronate or risedronate). Bisphosphonate treatment demonstrated limited effectiveness in preventing cortical bone microstructure deterioration with mechanical parameters remaining compromised due to CKD and/or secondary hyperparathyroidism irrespective of bisphosphonate treatment. •Single doses of zoledronate increased cortical porosity in two rodent models of CKD.•Fractionated bisphosphonate dosing did not affect cortical porosity.•Neither bisphosphonate regimen improved CKD-induced mechanical deficits.
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ISSN:2352-1872
2352-1872
DOI:10.1016/j.bonr.2022.101174