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1. A measure of intrinsic strength, not nominal strength, reflects effects of ex-vivo cortical bone matrix modulation by raloxifene

   https://doi.org/10.1016/j.jmbbm.2025.106956  

   Arnhart, Mary; Surowiec, Rachel K; Allen, Matthew R; Wallace, Joseph M; Pyrak-Nolte, Laura J; Howarter, John; Siegmund, Thomas (June 2025, Journal of the Mechanical Behavior of Biomedical Materials)

   Understanding bone strength is important when assessing bone diseases and their treatment. Bending experiments are often used to determine strength. Then, flexural stresses are calculated from elastic bending theory. With a brittle failure criterion, the maximum flexural tensile stress is equated to (nominal) strength. However, bone is not a perfectly brittle material. A quasi-brittle failure criterion is more appropriate. Such an approach allows for material failure to occur before full fracture. The extent of the subcritical damage domain then introduces a length scale. The intrinsic strength of the bone is calculated from the critical load at fracture and the failure process zone dimensions relative to the specimen size. We apply this approach to human cortical bone specimens extracted from a femur. We determine strength measures in the untreated reference state and after treatment with the selective estrogen receptor modulator raloxifene. We find that the common nominal strength measure does not distinguish between treatments. However, the dimensions of the failure process zone differ between treatments. Intrinsic strength measures then are demonstrated as descriptors of bone strength sensitive to treatment. An extrapolation of laboratory data to whole bone is demonstrated. 

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2. Load Data and Code for Analysis of In-situ X-ray Transverse Crack Growth Experiments in Specimens of a Human Cortical Bone

   https://doi.org/10.4231/RWPA-PG56  

   Gallaway, Glynn; Pyrak-Nolte, Laura; Siegmund, Thomas; Siegmund, Thomas (January 2025, Purdue University Research Repository)

   This publication documents measurement data for two in-situ loaded fracture mechanics specimens observed with 3D X-ray microscopy. Materials The diaphysis of a human (92-year-old, male) cadaveric femur was obtained through the Indiana University School of Medicine Anatomical Donation Program. Bars (nominally 4.0 mm x 4.0 mm cross section) were extracted from the diaphysis as demonstrated in Figure-samplelocation. Two single Edge Notch Bend, SEN(B), specimens for a load span s=20 mm were machined for a three-point bend fixture for crack growth in the transverse direction. SEN(B) specimens had the following dimensions (height d, depth b, initial crack length a0): beam 1 d=4.0 mm, b=4.0 mm, a0=1.8 mm, beam 2 d=4.1 mm, b=3.9 mm, a0=1.7 mm). Osteon diameter was measured was measured on polished sections by using backscatter SEM images following Britz (2009), Figure samplelocation.jpg. Using ImageJ, a grid is imposed on the images and On.Dm is determined as the Feret Diameter for at least 40 On.Dm measures. For beam 1 mean On.Dm is 242 micrometer and for beam 2 284 micrometer. Experiments and Data Fracture experiments were conducted with a Deben 5000 load rig in a Zeiss XRADIA 3D microscope. For system details see https://www.physics.purdue.edu/xrm/about-our-instruments/index.html. Data for these experiments is given in the two csv files of this project data set. In these experiments force F (load cell) data and image frame data are obtained as machine output. Crack mouth opening displacement (CMOD) is obtained from 3D X-ray images at frame numbers synchronized to force readings. Fracture process zone (FPZ) length L. FPZ length data is obtained from 3D image data in Gallaway, G. E.; Allen, M. R.; Surowiec, R. K.; Siegmund, T. H. (2025). 3D Image Data from In-situ X-ray Imaging Transverse Crack Growth Experiments in Human Cortical Bone. Purdue University Research Repository. doi:10.4231/94PZ-AB06 Code Code (Analysis_Main.m, Analysis_Func.m) takes data from the .csv files and determines the linear elastic fracture mechanics quantities (LEFM toughness), the quasi-brittle fracture mechanics quantities (QBFM toughness), and the tissue intrinsic (size-independent) fracture properties (tissue toughness, tissue strength, tissue lengthscale). Output is depicted as force-CMOD and fracture process zone length - CMOD records, and as crack growth resistance curves (quasibrittle energy release rate vs. fracture process zone length). In addition, the microstructure constant eta is obtained as the ratio between the tissue intrinsic lengthscale and the mean osteon diameter. Code (P_star.m) is provided to determine maximum sustainable load of a femoral shaft in three-point bending. It is assumed that the beam is a pipe with a surface crack of depth equal to the mean osteon diameter. This code can be used for sensitivity studies of the dependence of whole bone maximum sustainable load on cortical thickness, tissue intrinsic strength and microstructure constant eta. Example calculations are depicted in two relevant figures. 

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3. Germ‐Free C57BL /6 Mice Have Increased Bone Mass and Altered Matrix Properties but Not Decreased Bone Fracture Resistance

   https://doi.org/10.1002/jbmr.4835  

   Vahidi, Ghazal; Moody, Maya; Welhaven, Hope D.; Davidson, Leah; Rezaee, Taraneh; Behzad, Ramina; Karim, Lamya; Roggenbeck, Barbara A.; Walk, Seth T.; Martin, Stephen A.; et al (June 2023, Journal of Bone and Mineral Research)

   ABSTRACT The gut microbiome impacts bone mass, which implies a disruption to bone homeostasis. However, it is not yet clear how the gut microbiome affects the regulation of bone mass and bone quality. We hypothesized that germ‐free (GF) mice have increased bone mass and decreased bone toughness compared with conventionally housed mice. We tested this hypothesis using adult (20‐ to 21‐week‐old) C57BL/6J GF and conventionally raised female and male mice (n = 6–10/group). Trabecular microarchitecture and cortical geometry were measured from micro–CT of the femur distal metaphysis and cortical midshaft. Whole‐femur strength and estimated material properties were measured using three‐point bending and notched fracture toughness. Bone matrix properties were measured for the cortical femur by quantitative back‐scattered electron imaging and nanoindentation, and, for the humerus, by Raman spectroscopy and fluorescent advanced glycation end product (fAGE) assay. Shifts in cortical tissue metabolism were measured from the contralateral humerus. GF mice had reduced bone resorption, increased trabecular bone microarchitecture, increased tissue strength and decreased whole‐bone strength that was not explained by differences in bone size, increased tissue mineralization and fAGEs, and altered collagen structure that did not decrease fracture toughness. We observed several sex differences in GF mice, most notably for bone tissue metabolism. Male GF mice had a greater signature of amino acid metabolism, and female GF mice had a greater signature of lipid metabolism, exceeding the metabolic sex differences of the conventional mice. Together, these data demonstrate that the GF state in C57BL/6J mice alters bone mass and matrix properties but does not decrease bone fracture resistance. © 2023 The Authors.Journal of Bone and Mineral Researchpublished by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research (ASBMR). 

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4. Sex-specific effects of Fat-1 transgene on bone material properties, size, and shape in mice

   https://doi.org/10.1093/jbmrpl/ziad011  

   Bermudez, Beatriz; Brown, Kenna C.; Vahidi, Ghazal; Ferreira Ruble, Ana C.; Heveran, Chelsea M.; Ackert-Bicknell, Cheryl L.; Sherk, Vanessa D. (January 2024, JBMR Plus)

   Abstract Western diets are becoming increasingly common around the world. Western diets have high omega 6 (ω-6) and omega 3 (ω-3) fatty acids and are linked to bone loss in humans and animals. Dietary fats are not created equal; therefore, it is vital to understand the effects of specific dietary fats on bone. We aimed to determine how altering the endogenous ratios of ω-6:ω-3 fatty acids impacts bone accrual, strength, and fracture toughness. To accomplish this, we used the Fat-1 transgenic mice, which carry a gene responsible for encoding a ω-3 fatty acid desaturase that converts ω-6 to ω-3 fatty acids. Male and female Fat-1 positive mice (Fat-1) and Fat-1 negative littermates (WT) were given either a high-fat diet (HFD) or low-fat diet (LFD) at 4 wk of age for 16 wk. The Fat-1 transgene reduced fracture toughness in males. Additionally, male BMD, measured from DXA, decreased over the diet duration for HFD mice. In males, neither HFD feeding nor the presence of the Fat-1 transgene impacted cortical geometry, trabecular architecture, or whole-bone flexural properties, as detected by main group effects. In females, Fat-1-LFD mice experienced increases in BMD compared to WT-LFD mice; however, cortical area, distal femur trabecular thickness, and cortical stiffness were reduced in Fat-1 mice compared to pooled WT controls. However, reductions in stiffness were caused by a decrease in bone size and were not driven by changes in material properties. Together, these results demonstrate that the endogenous ω-6:ω-3 fatty acid ratio influences bone material properties in a sex-dependent manner. In addition, Fat-1 mediated fatty acid conversion was not able to mitigate the adverse effects of HFD on bone strength and accrual. 

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5. 3D Image Data from In-situ X-ray Imaging Transverse Crack Growth Experiments in Human Cortical Bone

   https://doi.org/10.4231/94PZ-AB06  

   Gallaway, Glynn; Allen, Matthew; Surowiec, Rachel; Siegmund, Thomas; Siegmund, Thomas H (January 2025, Purdue University Research Repository)

   This publication documents 3D image stacks from HR-pQCT imaging of a femur diaphysis, as well as image stacks for two in-situ loaded fracture mechanics specimens observed with 3D X-ray microscopy. Imaging For HR-qQCT: HR-pQCT scans were acquired by Rachel Surowiec using an XtremeCT II scanner (SCANCO Medical AG, Bruttisellen, Switzerland) within the Musculoskeletal Function, Imaging and Tissue (MSK-FIT) Resource Core of the Indiana Center for Musculoskeletal Health’s Clinical Research Center (Indiana University, Indianapolis, IN). Scans are performed at 60.7 um resolution, a 68 kV, 1467 uA, 43 ms integration time, 1 frame averaging. Raw scans are ‘.RSQ’ file types. The ISQ file type were read into ImageJ using the Import-KHKs Scanco uCT ISQ file reader plug-in, and exported as bmp image stacks, image stacks are provided in two parts. Reconstructed images are rotated in dataviewer so that all bones are in the same orientation (prox/distal/anterior/posterior for the Femur). For in-situ fracture mechanics experiments: 3D scans were acquired by Glynn Gallaway using a 3-point bending rig for single edged notched bend specimens with a Deben CT5000N load cell (Deben, Bury St. Edmunds, UK) in a Zeiss XRADIA 510 Versa 3D X-Ray microscope (Carl Zeiss AG, Baden-Württemberg, Germany) at Purdue University. The 3-point bending frame had a span 20 mm with X-ray transparent, glassy carbon supports. To maintain hydration, the beam was wrapped in a plastic film slit at the notch. Displacements were applied at 0.1 mm/min. Load cell outputs were monitored and recorded. Displacements are held constant during image acquisitions. The first 3D image was obtained at the onset of non-linearity. Subsequently, the displacement was increased until a load increase of 10 N was observed, and another image was obtained. This sequence was repeated 6-times until peak load. 3D X-ray images were acquired with a resolution of 4.5 um, exposure time 5 sec., 801 projections, 120 kV, 10 W, 4 x objective, and a LE2 filter. X-ray projections were processed through XRADIA Scout-and-Scan Reconstructor. A recursive Gaussian smoothing filter (s=1 pixel) was applied to reduce image artifacts. Image stacks are exported as tiff files and provided individually for each load step and specimen. Two experiments are documented (beam 1 and beam 2). MaterialstThe diaphysis of a human (92-year-old, male) cadaveric femur was obtained through the Indiana University School of Medicine Anatomical Donation Program. 

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