Abstract

The ability to rapidly screen animals for bone mineral content (BMC) and density (BMD) is of great importance. Recent advances in instrumentation, including dual-energy X-ray absorptiometry (DXA) and micro-computed tomography (uCT) have made it possible to determine BMC and BMD in vivo in small animal models. The proposed Small Animal Bone Phenotyping Core is a unique facility that has been developed by the Director, Dr. Timothy Nagy, to enable single projects to access state-of-the-art imaging techniques for the determination of BMC and BMD. The Core will provide all resources, including instrumentation and personnel, to carry out its mission. A centralized Core is required due to the cost of the instruments and the expertise required in their operations. The Director and personnel of the Core have demonstrated expertise in the effective use of this technology for the measurement of BMC and BMD in small animals, and are at the forefront of method development and validation of methods in this area. The Core will operate according to a formal quality assurance plan. In addition, the Core will provide extensive education in terms of the appropriate approaches, the limitations of the technology, and the interpretation of data. Extensive consultation on experimental design (especially animal housing and diet) also will be provided to ensure the generation of informative data.
Two specific aims are proposed for this interdisciplinary Core:
Specific Aim 1 : To provided accurate and precise measures of bone mineral content and density in small animal models. This will be accomplished by providing a centralized core facility containing stateof- the-art instrumentation (DXA and uCT) for in vivo and ex vivo bone imaging.
Specific Aim 2 : Validate new techniques and procedures that will enhance research in bone biology and allow investigators to ask novel questions while at the same time being assured of the resultant data. The Core has been strategically developed in response to investigator demand and has in the past 4 years supported 20 projects instigated by 13 past or current CCBSR investigators, including four Pilot and Feasibility study investigators. It has already stimulated innovative studies in the areas of basic bone cell biology as well as interdisciplinary studies in the area of the development of gene therapy for bone diseases. It is anticipated that its role in the CCBSR will expand considerably over the next 5 years given the enhanced access provided by the P30 funding mechanism, and the increasing use of small animal models by the CCBSR investigators. The Core complements the efforts of the other two CCBSR research Cores and several investigators use all three Cores in their ongoing studies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Center Core Grants (P30)
Project #
5P30AR046031-09
Application #
7880770
Study Section
Special Emphasis Panel (ZAR1)
Project Start
Project End
Budget Start
2009-06-01
Budget End
2010-05-31
Support Year
9
Fiscal Year
2009
Total Cost
$99,133
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Type
DUNS #
063690705
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Chen, Wei; Zhu, Guochun; Tang, Jun et al. (2018) C/ebp? controls osteoclast terminal differentiation, activation, function, and postnatal bone homeostasis through direct regulation of Nfatc1. J Pathol 244:271-282
Chen, Wei; Zhu, Guochun; Jules, Joel et al. (2018) Monocyte-Specific Knockout of C/ebp? Results in Osteopetrosis Phenotype, Blocks Bone Loss in Ovariectomized Mice, and Reveals an Important Function of C/ebp? in Osteoclast Differentiation and Function. J Bone Miner Res 33:691-703
Jules, Joel; Chen, Wei; Feng, Xu et al. (2018) C/EBP? transcription factor is regulated by the RANK cytoplasmic 535IVVY538 motif and stimulates osteoclastogenesis more strongly than c-Fos. J Biol Chem 293:1480-1492
Cai, Xiaofeng; Xing, Junjie; Long, Courtney L et al. (2017) DOK3 Modulates Bone Remodeling by Negatively Regulating Osteoclastogenesis and Positively Regulating Osteoblastogenesis. J Bone Miner Res 32:2207-2218
Wu, Mengrui; Wang, Yiping; Shao, Jian-Zhong et al. (2017) Cbf? governs osteoblast-adipocyte lineage commitment through enhancing ?-catenin signaling and suppressing adipogenesis gene expression. Proc Natl Acad Sci U S A 114:10119-10124
Jules, Joel; Chen, Wei; Feng, Xu et al. (2016) CCAAT/Enhancer-binding Protein ? (C/EBP?) Is Important for Osteoclast Differentiation and Activity. J Biol Chem 291:16390-403
Levy, Seth; Feduska, Joseph M; Sawant, Anandi et al. (2016) Immature myeloid cells are critical for enhancing bone fracture healing through angiogenic cascade. Bone 93:113-124
Higgs, Jerome T; Jarboe, John S; Lee, Joo Hyoung et al. (2015) Variants of Osteoprotegerin Lacking TRAIL Binding for Therapeutic Bone Remodeling in Osteolytic Malignancies. Mol Cancer Res 13:819-27
Li, Sheng; Hao, Liang; Wang, Lin et al. (2015) Targeting Atp6v1c1 Prevents Inflammation and Bone Erosion Caused by Periodontitis and Reveals Its Critical Function in Osteoimmunology. PLoS One 10:e0134903
Deshane, Jessy S; Redden, David T; Zeng, Meiqin et al. (2015) Subsets of airway myeloid-derived regulatory cells distinguish mild asthma from chronic obstructive pulmonary disease. J Allergy Clin Immunol 135:413-424.e15

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