Erythropoietin does not improve fracture healing in aged mice

Erythropoietin does not improve fracture healing in aged mice

Fracture healing in the elderly is associated with a declined healing potential caused by multiple factors including a delay of vascularization. Erythropoietin (EPO) has been demonstrated to improve vascularization and fracture healing in adult mice. We, therefore, hypothesized that EPO in aged mice...

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Published in:Experimental gerontology Vol. 122; pp. 1 - 9
Main Authors: Orth, M., Baudach, J., Scheuer, C., Osche, D., Veith, N.T., Braun, B.J., Rollmann, M.F., Herath, S.C., Pohlemann, T., Menger, M.D., Histing, T.
Format: Journal Article
Language:English
Published: England Elsevier Inc 15-07-2019
Subjects:
Aged mice
Bone healing
Bone turnover
EPO
Fracture healing
Tissue mineral density
Aged mice
Fracture healing
Bone healing
Bone turnover
Tissue mineral density
EPO
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Summary:Fracture healing in the elderly is associated with a declined healing potential caused by multiple factors including a delay of vascularization. Erythropoietin (EPO) has been demonstrated to improve vascularization and fracture healing in adult mice. We, therefore, hypothesized that EPO in aged mice also improves fracture healing. For this purpose, EPO was given daily in a femoral fracture model in aged mice and compared to vehicle-treated controls using radiological, biomechanical, histomorphometric and Western blot techniques. Blood analyses revealed significantly higher concentrations of hemoglobin and a higher hematocrit in EPO-treated animals at 14 and 35 days after fracture. Micro-computed tomography (μCT) indicated that the fraction of bone volume/tissue volume within the callus did not differ between the two groups. However, μCT showed a 3-fold increased tissue mineral density (TMD) in the callus of EPO-treated animals compared to controls. The callus TMD of the EPO-treated animals was also 2-fold higher when compared to the TMD of the unfractured contralateral femur. Interestingly, biomechanical analyses revealed a reduced bending stiffness in femurs of EPO-treated animals at day 35. The histomorphometrically analyzed callus size and callus composition did not show significant differences between the study groups. However, Western blot analyses exhibited an increased expression of osteoprotegerin (OPG), but in particular of receptor activator of NF-κB ligand (RANKL) in the callus of the EPO-treated animals. Further histological analyses of the callus tissue showed that this was associated with an increased number of newly formed blood vessels and a higher number of tartrate-resistant acid phosphatase (TRAP)+ cells. Conclusion: In fracture healing of aged mice EPO treatment increases callus TMD as well as OPG and RANKL expression, indicating an accelerated bone turnover when compared to controls. However, EPO does not improve fracture healing in aged mice. The process of fracture healing may be altered by EPO due to a deterioration of the microcirculation caused by the worsened rheological properties of the blood and due to an increased bone fragility caused by the accelerated bone turnover. Thus, EPO may not be used to improve fracture healing in the elderly. •EPO treatment increased hemoglobin, hematocrit and vascularization in aged mice.•EPO treatment increased tissue mineral density and reduced bending stiffness.•EPO-treated animals presented more osteoclasts and an accelerated bone turnover.•In contrast to young mice EPO may not be used to improve bone healing in the elderly.
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ISSN:0531-5565
1873-6815
DOI:10.1016/j.exger.2019.04.005