Abstract

? Immediately loaded orthopaedic and oral implants can undergo interfacial micromotion and fail by forming interfacial fibrous or cartilaginous tissue rather than bone. While in this instance and others it is evident that mechanical conditions affect healing of skeletal tissue (""""""""mechanobiology""""""""), specific factors influencing cell fate decisions, and mechanisms by which cells interpret and respond to changes in mechanical environment, remain unclear. This gap in understanding restricts design of conventional as well as new tissue-engineered implants. However, recent insights from fracture healing and other healing situations suggests the hypothesis that extracellular matrix remodeling and angiogenesis are central in bone healing around implants, and that tissue deformation (strain) during early implant loading affects these processes, and, in turn, cell differentiation at interfaces. To test this idea, this project will measure spatial/temporal expression of key molecular makers of angiogenesis, bone, and cartilage formation at: 1) healing sites without implants: and 2) healing interfaces where biomechanical strain conditions are varied. The project will use a novel model of the bone-implant interface in mouse tibiae, which allows experimental control of biomaterial and biomechanical factors. Also, the project will use wild-type (wt) and NEMP9-null mice (MMP9-/-), since the latter lack a key matrix metalloproteinase (MMP9, gelatinase B) involved in angiogenesis. The project will integrate data from in situ hybridization, ultrastructural analyses, immunocytochemistry and biomechanical tests to examine mechanobiology of interfacial healing.
Aim 1 will test if matrix remodeling and angiogenesis are prerequisites for osteoblast (OB) differentiation in holes without implants;
the aim will develop a """"""""molecular map"""""""" of expression of markers of angiogenesis, bone and cartilage formation during healing of empty drill holes (diam. 0.2, 0.4 and 1.0 ram) at 3, 9 and 27 days in wt and MMP9-/- mice.
Aim 2 will test if matrix remodeling and angiogenesis are essential for differentiation of mesenchymal cells into OBs in unstrained bone-implant gaps. Using wt and MMP9-/- mice, we will develop molecular maps of healing at 0, 3, 9 and 27 days at: (1) a bone-implant gap interface (BIGI) around stabilized polylactide (PLA) pins in oversized holes; and (2) a direct bone-implant interface (DBII), having a mix of direct bone-implant contact and gaps around stabilized PLA screws.
Aim 3 will control implant micromotion in its implant bed, in response to a defined load immediately post-implantation, to test whether specific strain conditions in interfacial gaps inhibit matrix remodeling, angiogenesis and differentiation of mesenchymal cells into OBs. A miniaturized rmcromotion device will be used to create implant stability vs. cyclic axial implant micromotion (100-200 (m) of pins and screws in a BIGI during healing. Interfaces will be analyzed biologically as in Aims 1-2, and interfacial strain fields will be measured directly by digital image correlation based on micro-CT images of whole bone-implant specimens. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Biomedical Imaging and Bioengineering (NIBIB)
Type
Research Project (R01)
Project #
5R01EB000504-04
Application #
7037636
Study Section
Special Emphasis Panel (ZRG1-SSS-M (01))
Program Officer
Henderson, Lori
Project Start
2003-07-01
Project End
2008-04-30
Budget Start
2006-05-01
Budget End
2008-04-30
Support Year
4
Fiscal Year
2006
Total Cost
$464,619
Indirect Cost

  Institution

Name
Rensselaer Polytechnic Institute
Department
Biomedical Engineering
Type
Schools of Engineering
DUNS #
002430742
City
Troy
State
NY
Country
United States
Zip Code
12180

  Publications

Haïat, Guillaume; Wang, Hom-Lay; Brunski, John (2014) Effects of biomechanical properties of the bone-implant interface on dental implant stability: from in silico approaches to the patient's mouth. Annu Rev Biomed Eng 16:187-213
Lim, Won Hee; Liu, Bo; Cheng, Du et al. (2014) Wnt signaling regulates pulp volume and dentin thickness. J Bone Miner Res 29:892-901
Mouraret, S; Hunter, D J; Bardet, C et al. (2014) A pre-clinical murine model of oral implant osseointegration. Bone 58:177-84
Mouraret, Sylvain; Hunter, Daniel J; Bardet, Claire et al. (2014) Improving oral implant osseointegration in a murine model via Wnt signal amplification. J Clin Periodontol 41:172-80
Li, Jingtao; Johnson, Chelsey A; Smith, Andrew A et al. (2014) Molecular mechanisms underlying skeletal growth arrest by cutaneous scarring. Bone 66:223-31
Wazen, Rima M; Kuroda, Shingo; Nishio, Clarice et al. (2013) Gene expression profiling and histomorphometric analyses of the early bone healing response around nanotextured implants. Nanomedicine (Lond) 8:1385-95
Leucht, P; Monica, S D; Temiyasathit, S et al. (2013) Primary cilia act as mechanosensors during bone healing around an implant. Med Eng Phys 35:392-402
Wazen, Rima M; Currey, Jennifer A; Guo, Hongqiang et al. (2013) Micromotion-induced strain fields influence early stages of repair at bone-implant interfaces. Acta Biomater 9:6663-74
Variola, Fabio; Brunski, John B; Orsini, Giovanna et al. (2011) Nanoscale surface modifications of medically relevant metals: state-of-the art and perspectives. Nanoscale 3:335-53
Popelut, Antoine; Rooker, Scott M; Leucht, Philipp et al. (2010) The acceleration of implant osseointegration by liposomal Wnt3a. Biomaterials 31:9173-81

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