TY - JOUR
T1 - Quantitative measures of femoral fracture repair in rats derived by micro-computed tomography
AU - Nyman, Jeffry S.
AU - Munoz, Steve
AU - Jadhav, Satyawan
AU - Mansour, Alfred
AU - Yoshii, Toshitaka
AU - Mundy, Gregory R.
AU - Gutierrez, Gloria E.
PY - 2009/5/11
Y1 - 2009/5/11
N2 - Although fracture healing is frequently studied in pre-clinical models of long bone fractures using rodents, there is a dearth of objective quantitative techniques to assess successful healing. Biomechanical testing is possibly the most quantitative and relevant to a successful clinical outcome, but it is a destructive technique providing little insight into the cellular mechanisms associated with healing. The advent of X-ray computed tomography (CT) has provided the opportunity to quantitatively and non-destructively assess bone structure and density, but it is unknown how measurements derived using this technology relate to successful healing. To examine possible relationships, we used a pre-clinical model to test for statistically significant correlations between quantitative characteristics of the callus by micro-CT (μCT) and the bending strength, stiffness, and energy-to-failure of the callus as assessed by three-point bending of excised bones. A closed, transverse fracture was generated in the mid-shaft of rat femurs by impact loading. Shortly thereafter, the rats received a one-time, local injection of either the vehicle or one of four doses of lovastatin. Following sacrifice after 4 weeks of healing, fractured femurs were extracted for μCT analysis and then three-point bending. Setting the region of interest to be 3.2 mm above and below the fracture line, we acquired standard and new μCT-derived measurements. The mineralized callus volume and the mineral density of the callus correlated positively with callus strength (rxy=-0.315, p=0.016 and rxy=0.444, p<0.0005, respectively) and stiffness (rxy=-0.271, p=0.040 and rxy=0.325, p=0.013, respectively), but the fraction of the callus that mineralized and the moment of inertia of the callus did not. This fraction did correlate with energy-to-failure (rxy=-0.343, p=0.0085). Of the μCT-derived measurements, quantifying defects within the outer bridging cortices of the callus produced the strongest correlation with both callus strength (rxy=0.557, p<0.0001) and stiffness (rxy=0.468, p=0.0002). By both reducing structural defects and increasing mineralization, lovastatin appears to increase the callus strength.
AB - Although fracture healing is frequently studied in pre-clinical models of long bone fractures using rodents, there is a dearth of objective quantitative techniques to assess successful healing. Biomechanical testing is possibly the most quantitative and relevant to a successful clinical outcome, but it is a destructive technique providing little insight into the cellular mechanisms associated with healing. The advent of X-ray computed tomography (CT) has provided the opportunity to quantitatively and non-destructively assess bone structure and density, but it is unknown how measurements derived using this technology relate to successful healing. To examine possible relationships, we used a pre-clinical model to test for statistically significant correlations between quantitative characteristics of the callus by micro-CT (μCT) and the bending strength, stiffness, and energy-to-failure of the callus as assessed by three-point bending of excised bones. A closed, transverse fracture was generated in the mid-shaft of rat femurs by impact loading. Shortly thereafter, the rats received a one-time, local injection of either the vehicle or one of four doses of lovastatin. Following sacrifice after 4 weeks of healing, fractured femurs were extracted for μCT analysis and then three-point bending. Setting the region of interest to be 3.2 mm above and below the fracture line, we acquired standard and new μCT-derived measurements. The mineralized callus volume and the mineral density of the callus correlated positively with callus strength (rxy=-0.315, p=0.016 and rxy=0.444, p<0.0005, respectively) and stiffness (rxy=-0.271, p=0.040 and rxy=0.325, p=0.013, respectively), but the fraction of the callus that mineralized and the moment of inertia of the callus did not. This fraction did correlate with energy-to-failure (rxy=-0.343, p=0.0085). Of the μCT-derived measurements, quantifying defects within the outer bridging cortices of the callus produced the strongest correlation with both callus strength (rxy=0.557, p<0.0001) and stiffness (rxy=0.468, p=0.0002). By both reducing structural defects and increasing mineralization, lovastatin appears to increase the callus strength.
KW - Biomechanics
KW - Fracture healing
KW - Micro-CT
KW - Rat
KW - Statin
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UR - http://www.scopus.com/inward/citedby.url?scp=64549142793&partnerID=8YFLogxK
U2 - 10.1016/j.jbiomech.2009.01.016
DO - 10.1016/j.jbiomech.2009.01.016
M3 - Article
C2 - 19281987
AN - SCOPUS:64549142793
SN - 0021-9290
VL - 42
SP - 891
EP - 897
JO - Journal of Biomechanics
JF - Journal of Biomechanics
IS - 7
ER -