Your search keyword '"Jennifer A. McKenzie"' showing total 8 results

1. VEGFA from osteoblasts is not required for lamellar bone formation following tibial loading

Author

Jennifer A. McKenzie, Ian M. Galbreath, Andre F. Coello, Katherine R. Hixon, and Matthew J. Silva

Subjects

Male, Vascular Endothelial Growth Factor A, Mice, Histology, Osteoblasts, Tibia, Physiology, Osteogenesis, Endocrinology, Diabetes and Metabolism, Animals, Female, Bone and Bones

Abstract

The relationship between osteogenesis and angiogenesis is complex. Normal bone development requires angiogenesis, mediated by vascular endothelial growth factor A (VEGFA). Studies have demonstrated through systemic inhibition or genetic modification that VEGFA is indispensable for several types of bone repair, presumably via its role in supporting angiogenesis. But a direct role for VEGFA within osteoblasts, in the absence of angiogenesis, has also been suggested. To address the question of whether VEGFA from osteoblasts supports bone formation directly, we applied anabolic loading to induce lamellar bone formation in mice, a process shown to be independent of angiogenesis. We hypothesized that VEGFA from osteoblasts is required for lamellar bone formation. To test this hypothesis, we applied axial tibial compression to inducible Cre/LoxP mice from three lines. Vegfa

Published

2022

2. Exogenous hedgehog antagonist delays but does not prevent fracture healing in young mice

Author

Michael J. Gardner, Xiaochen Liu, Clayton W. Maschhoff, Jennifer A. McKenzie, and Matthew J. Silva

Subjects

0301 basic medicine, Aging, medicine.medical_specialty, Histology, Pyridines, Physiology, Angiogenesis, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Bone healing, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, GLI1, Internal medicine, medicine, Animals, Anilides, Hedgehog Proteins, Endochondral ossification, Fracture Healing, biology, business.industry, Chondrogenesis, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Callus, biology.protein, Female, Cortical bone, Smoothened, business, Signal Transduction

Abstract

Fracture healing recapitulates many aspects of developmental osteogenesis. The hedgehog (Hh) signaling pathway, essential to skeletal development, is upregulated during fracture healing, although its importance is unclear. Our goal was to assess the functional importance of Hh signaling in endochondral fracture healing. We created closed, transverse diaphyseal femur fractures in mice, stabilized with an intramedullary pin, and administered a systemic Hh inhibitor or vehicle. Because Hh pathway activation is mediated by the receptor Smoothened (Smo), we used the Smo antagonist GDC-0449 (GDC, 50 mg/kg, twice daily) to target the pathway. First, in vehicle-treated 10-wk. female C57BL/6 mice we confirmed that Hh signaling was increased in fracture callus compared to intact bone, with > 5-fold upregulation of target genes Ptch1 and Gli1 . Additionally, using 10-wk. male and female Gli1 reporter mice, we saw a strong activation of the reporter in the osseous regions of the fracture callus 7–10 days after fracture. GDC treatment significantly blunted these responses, indicating effective inhibition of fracture-induced Hh signaling in bone. Moreover, microCT analysis revealed that GDC treatment significantly reduced cancellous and cortical bone volume at non-fracture sites (tibial metaphysis and diaphysis), suggesting that the drug inhibited normal bone formation. GDC treatment had a modest effect on fracture healing, with evidence of delayed callus mineralization radiographically (significantly lower Goldberg score at day 14) and by microCT (reduced callus vBMD at 14 days), and a delay in the recovery of torsional rotation to normal (elevated rotation-at-peak torque at 21 days). On the other hand, GDC treatment did not inhibit qPCR or morphological measures of chondrogenesis or angiogenesis, and did not impair the recovery of failure torque (at day 14 or 21), a measure of biomechanical competence. In summary, GDC treatment inhibited Hh signaling, which delayed but did not prevent fracture healing in young mice. We conclude that Hh signaling is strongly induced after fracture and may play a role in early callus mineralization, although it does not appear to be required for eventual healing.

Published

2017

3. Transcriptional profiling of intramembranous and endochondral ossification after fracture in mice

Author

Evan G. Buettmann, Paul Gontarz, Jennifer A. McKenzie, Bo Zhang, Matthew J. Silva, Brandon A. Coates, and Xiaochen Liu

Subjects

0301 basic medicine, Histology, Fractures, Stress, Transcription, Genetic, Physiology, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Bone healing, Biology, Article, Transcriptome, 03 medical and health sciences, Fractures, Bone, 0302 clinical medicine, Downregulation and upregulation, Osteogenesis, Gene expression, medicine, Animals, RNA-Seq, Bony Callus, Endochondral ossification, Gene, Fracture Healing, Principal Component Analysis, Membranes, Gene Expression Profiling, Reproducibility of Results, Bone fracture, medicine.disease, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Gene Ontology, Phenotype, Gene Expression Regulation, Intramembranous ossification, Disease Progression, Female

Abstract

Bone fracture repair represents an important clinical challenge with nearly 1 million non-union fractures occurring annually in the U.S. Gene expression differs between non-union and healthy repair, suggesting there is a pattern of gene expression that is indicative of optimal repair. Despite this, the gene expression profile of fracture repair remains incompletely understood. In this work, we used RNA-seq of two well-established murine fracture models to describe gene expression of intramembranous and endochondral bone formation. We used top differentially expressed genes, enriched gene ontology terms and pathways, callus cellular phenotyping, and histology to describe and contrast these bone formation processes across time. Intramembranous repair, as modeled by ulnar stress fracture, and endochondral repair, as modeled by femur full fracture, exhibited vastly different transcriptional profiles throughout repair. Stress fracture healing had enriched differentially expressed genes associated with bone repair and osteoblasts, highlighting the strong osteogenic repair process of this model. Interestingly, the PI3K-Akt signaling pathway was one of only a few pathways uniquely enriched in stress fracture repair. Full fracture repair involved a higher level of inflammatory and immune cell related genes than did stress fracture repair. Full fracture repair also differed from stress fracture in a robust downregulation of ion channel genes following injury, the role of which in fracture repair is unclear. This study offers a broad description of gene expression in intramembranous and endochondral ossification across several time points throughout repair and suggests several potentially intriguing genes, pathways, and cells whose role in fracture repair requires further study.

Published

2019

4. Type 1 diabetic Akita mice have low bone mass and impaired fracture healing

Author

Evan G. Buettmann, Pei Hu, Jennifer A. McKenzie, Michael J. Gardner, Nicole Migotsky, and Matthew J. Silva

Subjects

0301 basic medicine, endocrine system, medicine.medical_specialty, Histology, endocrine system diseases, Physiology, Endocrinology, Diabetes and Metabolism, Low bone mass, 030209 endocrinology & metabolism, Bone healing, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Diabetes mellitus, medicine, Animals, Bone formation, Femur, Bony Callus, Fracture Healing, Femur fracture, business.industry, Cartilage, Wild type, medicine.disease, Diabetes Mellitus, Type 1, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, business, Femoral Fractures, hormones, hormone substitutes, and hormone antagonists

Abstract

Type 1 diabetes (T1DM) impairs bone formation and fracture healing in humans. Akita mice carry a mutation in one allele of the insulin-2 (Ins2) gene, which leads to pancreatic beta cell dysfunction and hyperglycemia by 5–6 weeks age. We hypothesized that T1DM in Akita mice is associated with decreased bone mass, weaker bones, and impaired fracture healing. Ins2 +/− (Akita) and wildtype (WT) males were subjected to femur fracture at 18-weeks age and healing assessed 3–21 days post-fracture. Non-fractured left femurs were assessed for morphology (microCT) and strength (bending or torsion) at 19–21 weeks age. Fractured right femurs were assessed for callus mechanics (torsion), morphology and composition (microCT and histology) and gene expression (qPCR). Both Akita and WT mice gained weight from 3 to 18 weeks age, but Akita mice weighed less starting at 5 weeks (−5.2%, p < 0.05). At 18–20 weeks age Akita mice had reduced serum osteocalcin (−30%), cortical bone area (−16%), and thickness (−17%) compared to WT, as well as reduced cancellous BV/TV (−39%), trabecular thickness (−23%) and vBMD (−31%). Mechanical testing of non-fractured femurs showed decreased structural (stiffness, ultimate load) and material (ultimate stress) properties of Akita bones. At 14 and 21 days post fracture Akita mice had a significantly smaller callus than WT mice (~30%), with less cartilage and bone area. Assessment of torsional strength showed a weaker callus in Akita mice with lower stiffness (−42%), maximum torque (−44%) and work to fracture (−44%). In summary, cortical and cancellous bone mass were reduced in Akita mice, with lower bone mechanical properties. Fracture healing in Akita mice was impaired by T1DM, with a smaller, weaker fracture callus due to decreased cartilage and bone formation. In conclusion, the Akita mouse mimics some of the skeletal features of T1DM in humans, including osteopenia and impaired fracture healing, and may be useful to test interventions.

Published

2021

5. Bmp2 conditional knockout in osteoblasts and endothelial cells does not impair bone formation after injury or mechanical loading in adult mice

Author

Jennifer A. McKenzie, Sarah McBride-Gagyi, Evan G. Buettmann, Michael J. Gardner, and Matthew J. Silva

Subjects

Male, animal structures, Histology, Fractures, Stress, Physiology, Endocrinology, Diabetes and Metabolism, Bone Morphogenetic Protein 2, Gene Expression, Bone healing, Bone morphogenetic protein 2, Article, Mice, Osteogenesis, Conditional gene knockout, Bone cell, Animals, Endochondral ossification, Fracture Healing, Mice, Knockout, Femur fracture, Osteoblasts, Chemistry, Bone Injury, fungi, Endothelial Cells, Anatomy, biological factors, Cell biology, embryonic structures, Intramembranous ossification, Female, Stress, Mechanical

Abstract

Post-natal osteogenesis after mechanical trauma or stimulus occurs through either endochondral healing, intramembranous healing or lamellar bone formation. Bone morphogenetic protein 2 (BMP2) is up-regulated in each of these osteogenic processes and is expressed by a variety of cells including osteoblasts and vascular cells. It is known that genetic knockout of Bmp2 in all cells or in osteo-chondroprogenitor cells completely abrogates endochondral healing after full fracture. However, the importance of BMP2 from differentiated osteoblasts and endothelial cells is not known. Moreover, the importance of BMP2 in non-endochondral bone formation such as intramembranous healing or lamellar bone formation is not known. Using inducible and tissue-specific Cre-lox mediated targeting of Bmp2 in adult (10-24 week old) mice, we assessed the role of BMP2 expression globally, by osteoblasts, and by vascular endothelial cells in endochondral healing, intramembranous healing and lamellar bone formation. These three osteogenic processes were modeled using full femur fracture, ulnar stress fracture, and ulnar non-damaging cyclic loading, respectively. Our results confirmed the requirement of BMP2 for endochondral fracture healing, as mice in which Bmp2 was knocked out in all cells prior to fracture failed to form a callus. Targeted deletion of Bmp2 in osteoblasts (osterix-expressing) or vascular endothelial cells (vascular endothelial cadherin-expressing) did not impact fracture healing in any way. Regarding non-endochondral bone formation, we found that BMP2 is largely dispensable for intramembranous bone formation after stress fracture and also not required for lamellar bone formation induced by mechanical loading. Taken together our results indicate that osteoblasts and endothelial cells are not a critical source of BMP2 in endochondral fracture healing, and that non-endochondral bone formation in the adult mouse is not as critically dependent on BMP2.

Published

2015

6. Hedgehog signaling mediates woven bone formation and vascularization during stress fracture healing

Author

Fanxin Long, Jennifer A. McKenzie, Nikolas H. Kazmers, Tony S. Shen, and Matthew J. Silva

Subjects

Male, medicine.medical_specialty, Histology, Fractures, Stress, Pyridines, Physiology, Angiogenesis, Endocrinology, Diabetes and Metabolism, Neovascularization, Physiologic, Bone healing, Article, Bone resorption, Osteogenesis, Internal medicine, medicine, Animals, Anilides, Hedgehog Proteins, Bone Resorption, Cell Proliferation, Fracture Healing, biology, Chemistry, ALPL, Rats, Inbred F344, Hedgehog signaling pathway, Rats, Up-Regulation, Apposition, Endocrinology, RANKL, Callus, biology.protein, Signal Transduction

Abstract

Hedgehog (Hh) signaling is critical in developmental osteogenesis, and recent studies suggest it may also play a role in regulating osteogenic gene expression in the post-natal setting. However, there is a void of studies directly assessing the effect of Hh inhibition on post-natal osteogenesis. This study utilized a cyclic loading-induced ulnar stress fracture model to evaluate the hypothesis that Hh signaling contributes to osteogenesis and angiogenesis during stress fracture healing. Immediately prior to loading, adult rats were given GDC-0449 (Vismodegib - a selective Hh pathway inhibitor; 50mg/kg orally twice daily), or vehicle. Hh signaling was upregulated in response to stress fracture at 3 days (Ptch1, Gli1 expression), and was markedly inhibited by GDC-0449 at 1 day and 3 days in the loaded and non-loaded ulnae. GDC-0449 did not affect Hh ligand expression (Shh, Ihh, Dhh) at 1 day, but decreased Shh expression by 37% at 3 days. GDC-0449 decreased woven bone volume (-37%) and mineral density (-17%) at 7 days. Dynamic histomorphometry revealed that the 7 day callus was composed predominantly of woven bone in both groups. The observed reduction in woven bone occurred concomitantly with decreased expression of Alpl and Ibsp, but was not associated with differences in early cellular proliferation (as determined by callus PCNA staining at 3 days), osteoblastic differentiation (Osx expression at 1 day and 3 days), chondrogenic gene expression (Acan, Sox9, and Col2α1 expression at 1 day and 3 days), or bone resorption metrics (callus TRAP staining at 3 days, Rankl and Opg expression at 1 day and 3 days). To evaluate angiogenesis, vWF immunohistochemistry showed that GDC-0449 reduced fracture callus blood vessel density by 55% at 3 days, which was associated with increased Hif1α gene expression (+30%). Dynamic histomorphometric analysis demonstrated that GDC-0449 also inhibited lamellar bone formation. Lamellar bone analysis of the loaded limb (directly adjacent to the woven bone callus) showed that GDC-0449 significantly decreased mineral apposition rate (MAR) and bone formation rate (BFR/BS) (-17% and -20%, respectively). Lamellar BFR/BS in the non-loaded ulna was also significantly decreased (-37%), indicating that Hh signaling was required for normal bone modeling. In conclusion, Hh signaling plays an important role in post-natal osteogenesis in the setting of stress fracture healing, mediating its effects directly through regulation of bone formation and angiogenesis.

Published

2015

7. Healing of non-displaced fractures produced by fatigue loading of the mouse ulna

Author

David M. Ornitz, Jennifer A. McKenzie, Matthew J. Silva, Gregory J. Schmid, and Mario D. Martinez

Subjects

Male, Histology, Compressive Strength, Physiology, Medial cortex, Sialoglycoproteins, Endocrinology, Diabetes and Metabolism, Bone Morphogenetic Protein 2, Ulna, Bone healing, Article, Mice, medicine, Animals, Integrin-Binding Sialoprotein, Displacement (orthopedic surgery), Fracture Healing, Reverse Transcriptase Polymerase Chain Reaction, business.industry, Cartilage, Anatomy, Hypoxia-Inducible Factor 1, alpha Subunit, Ulna Fractures, Skeleton (computer programming), Biomechanical Phenomena, Mice, Inbred C57BL, medicine.anatomical_structure, Forelimb, Tomography, X-Ray Computed, business

Abstract

We developed a fatigue loading protocol in mice to produce a non-displaced ulnar fracture in vivo, and characterized the early healing response. Using adult (5 month) C57Bl/6 mice, we first determined that cyclic compression of the forelimb under load-control leads to increasing applied displacement and, eventually, complete fracture. We then subjected the right forelimbs of 80 mice to cyclic loading (2 Hz; peak force approximately 4N) and limited the displacement increase to 0.75 mm (60% of the average displacement increase at complete fracture). This fatigue protocol created a partial, non-displaced fracture through the medial cortex near the ulnar mid-shaft, and reduced ulnar strength and stiffness by >50%. Within 1 day, there was significant upregulation of genes related to hypoxia (Hif1a) and osteogenesis (Bmp2, Bsp) in loaded ulnae compared to non-loaded, contralateral controls. The gene expression response peaked in magnitude near day 7 (e.g., Osx upregulated 8-fold), and included upregulation of FGF-family genes (e.g., Fgfr3 up 6-fold). Histologically, a localized periosteal response was seen at the site of the fracture; by day 7 there was abundant periosteal woven bone surrounding a region of cartilage. From days 7 to 14, the woven bone became denser but did not increase in area. By day 14, the woven-bone response resulted in complete recovery of ulnar strength and stiffness, restoring mechanical properties to normal levels. In the future, the fatigue loading approach can be used create non-displaced bone fractures in transgenic and knockout mice to study the mechanisms by which the skeleton rapidly repairs damage.

Published

2010

8. Angiogenesis is required for stress fracture healing in rats

Author

Anne H. Schmieder, Ryan E. Tomlinson, Matthew J. Silva, Jennifer A. McKenzie, Gregory M. Lanza, and Gregory R. Wohl

Subjects

Male, Pathology, medicine.medical_specialty, Histology, Fractures, Stress, Physiology, Angiogenesis, Endocrinology, Diabetes and Metabolism, Neovascularization, Physiologic, Bone healing, Article, Vascularity, Medicine, Animals, Fumagillin, Fracture Healing, Stress fractures, business.industry, Endoglin, medicine.disease, Immunohistochemistry, Rats, Inbred F344, Rats, medicine.anatomical_structure, medicine.symptom, Forelimb, business, medicine.drug

Abstract

Although angiogenesis and osteogenesis are critically linked, the importance of angiogenesis for stress fracture healing is unknown. In this study, mechanical loading was used to create a non-displaced stress fracture in the adult rat forelimb. Fumagillin, an anti-angiogenic agent, was used as the water soluble analogue TNP-470 (25mg/kg) as well as incorporated into lipid-encapsulated α(v)β(3) integrin targeted nanoparticles (0.25mg/kg). In the first experiment, TNP-470 was administered daily for 5 days following mechanical loading, and changes in gene expression, vascularity, and woven bone formation were quantified. Although no changes in vascularity were detected 3 days after loading, treatment-related downregulation of angiogenic (Pecam1) and osteogenic (Bsp, Osx) genes was observed at this early time point. On day 7, microCT imaging of loaded limbs revealed diminished woven bone formation in treated limbs compared to vehicle treated limbs. In the second experiment, α(v)β(3) integrin targeted fumagillin nanoparticles were administered as before, albeit with a 100-fold lower dose, and changes in vascularity and woven bone formation were determined. There were no treatment-related changes in vessel count or volume 3 days after loading, although fewer angiogenic (CD105 positive) blood vessels were present in treated limbs compared to vehicle treated limbs. This result manifested on day 7 as a reduction in total vascularity, as measured by histology (vessel count) and microCT (vessel volume). Similar to the first experiment, treated limbs had diminished woven bone formation on day 7 compared to vehicle treated limbs. These results indicate that angiogenesis is required for stress fracture healing, and may have implications for inducing rapid repair of stress fractures.

Published

2012