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Determining elemental strontium distribution in...
Journal article

Determining elemental strontium distribution in rat bones treated with strontium ranelate and strontium citrate using 2D micro‐XRF and 3D dual energy K‐edge subtraction synchrotron imaging

Abstract

Strontium‐based medications, such as strontium ranelate, have been suggested to have therapeutic effects in patients with osteoporosis. Strontium salts available off‐shelf in stores across North America are assumed to provide similar effects as strontium ranelate and thus should lead to similar distributions of elemental strontium incorporated in bone. The objective of this study was to compare the spatial distribution of strontium in animal bones following the administration of strontium ranelate and strontium citrate. Seventeen‐week‐old Sprague–Dawley rats were split into three groups over 10 weeks and given 625 mg/kg/day of strontium ranelate and 676 mg/kg/day of strontium citrate; the control group received no additional supplementary strontium. The humeri were collected from all animals, and strontium distribution was mapped using 2D micro‐XRF and 3D dual energy K‐edge subtraction (KES) imaging. 2D and 3D elemental mapping methods demonstrated that strontium delivered during treatment by both salts had the same spatial distribution. 3D elemental strontium maps of treated animal bones showed that strontium was largely observed in the trabecular regions under the epiphyseal (growth) plate. The thickness of the strontium layers in both the strontium ranelate and strontium citrate sample was not significantly different ( p = .9201). 2D micro‐XRF and 3D dual‐energy KES images effectively elucidated the spatial distribution of elemental strontium in calcified tissue. These methods provide a novel approach to evaluating the potential efficacy of strontium supplements in the treatment of osteoporosis.

Authors

Cardenas D; Turyanskaya A; Rauwolf M; Panahifar A; Cooper D; Wohl GR; Streli C; Wobrauschek P; Pejović‐Milić A

Journal

X-Ray Spectrometry, Vol. 49, No. 3, pp. 424–433

Publisher

Wiley

Publication Date

May 1, 2020

DOI

10.1002/xrs.3127

ISSN

0049-8246

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