Total joint replacement (TJR) is a highly successful surgical procedure, however the long-term survivorship is limited by wear of the bearing surfaces. In vitro, in vivo and tissue retrieval studies have demonstrated a critical role for Monocyte Chemoattractant Protein-1 (MCP-1) in wear particle-induced inflammation. The goals of this grant proposal are twofold 1) to develop, functionalize and validate a novel orthopaedic implant nano-coating that will deliver anti-MCP-1 protein therapy to the implant-bone interface and 2) to modulate macrophage polarization at the interface from an M1 (pro-inflammatory) to an M2 (pro-tissue remodeling and angiogenesis) phenotype with local infusion of the anti-inflammatory cytokine Interleukin-4 (IL-4). Both of these strategies will decrease chronic inflammation near the implant, improve bone apposition, and decrease particle-induced bone loss due to continuous local infusion of wear particles using our established in vivo murine model.
Specific Aim #1 : To construct, optimize and validate a local delivery system in which mutant anti-MCP-1 protein (known as 7ND protein) is eluted from a titanium rod in vitro.
Specific Aim #2 : To demonstrate that local delivery of 7ND protein decreases systemic macrophage trafficking to the protein eluting titanium implant, thereby improving bone apposition and decreasing peri- implant osteolysis, using the murine continuous polyethylene particle infusion model.
Specific Aim #3 : To demonstrate that transformation of macrophages located at the bone-implant interface in the presence of continuously infused polyethylene particles from a M1 (pro-inflammatory) to a M2 (pro-tissue remodeling and angiogenesis) phenotype with local delivery of IL-4 will decrease bone loss and improve bone apposition adjacent to the implant.
Specific Aim #4 : To demonstrate using biomechanical evaluation that coating titanium implants with 7ND protein or local delivery of IL-4 improves implant fixation and bone structural properties in the presence of continuously infused polyethylene particles. The proposed studies aspire to modulate the inflammatory reaction to polymer wear particles using a murine model of continuous polyethylene particle infusion, similar to the clinical scenario in humans. Strategies which target macrophage migration (delivery of a mutant MCP-1 protein near the implant) and alter the phenotype of local peri-implant macrophages to one supporting tissue remodeling and angiogenesis (local infusion of IL-4) will be tested. Imaging, histology, morphometry, and mechanical testing will be used to delineate systemic trafficking of macrophages to the particles, the characteristics of the local inflammatory reaction, and development or prevention of osteolysis. The biological strategies proposed are novel, mechanistic and directly translational;they should result in decreased peri-implant inflammation, enhanced bone apposition, decreased particle-induced bone loss and improved biomechanical properties, potentially extending the lifetime of TJRs.

Public Health Relevance

Total joint replacement (TJR) is a highly successful surgical procedure for end-stage arthritis, however the longevity of TJRs is limited by wear of the bearing surfaces. Wear particles stimulate a chronic inflammatory reaction that causes local bone destruction around the implant. The purpose of this grant is to test two novel translational strategies to mitigate particle-associated bone destruction by interfering with inflammatory cell signaling, and transforming the inflammatory cells to cells favoring tissue regeneration. Both strategies have a high likelihood of extending the lifetime of TJRs in humans.

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
3R01AR055650-07S1
Application #
8762272
Study Section
Musculoskeletal Tissue Engineering Study Section (MTE)
Program Officer
Panagis, James S
Project Start
2007-09-15
Project End
2015-08-31
Budget Start
2014-09-05
Budget End
2015-08-31
Support Year
7
Fiscal Year
2014
Total Cost
$176,781
Indirect Cost
$66,779
Name
Stanford University
Department
Surgery
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305
Chan, Charles K F; Gulati, Gunsagar S; Sinha, Rahul et al. (2018) Identification of the Human Skeletal Stem Cell. Cell 175:43-56.e21
Pajarinen, Jukka; Lin, Tzu-Hua; Goodman, Stuart B (2018) Production of GFP and Luciferase-Expressing Reporter Macrophages for In Vivo Bioluminescence Imaging. Methods Mol Biol 1790:99-111
Lin, Tzuhua; Kohno, Yusuke; Huang, Jhih-Fong et al. (2018) NF?B sensing IL-4 secreting mesenchymal stem cells mitigate the proinflammatory response of macrophages exposed to polyethylene wear particles. J Biomed Mater Res A 106:2744-2752
Pajarinen, Jukka; Lin, Tzuhua; Gibon, Emmanuel et al. (2018) Mesenchymal stem cell-macrophage crosstalk and bone healing. Biomaterials :
Lin, Tzuhua; Pajarinen, Jukka; Nabeshima, Akira et al. (2017) Preconditioning of murine mesenchymal stem cells synergistically enhanced immunomodulation and osteogenesis. Stem Cell Res Ther 8:277
Gibon, Emmanuel; Amanatullah, Derek F; Loi, Florence et al. (2017) The biological response to orthopaedic implants for joint replacement: Part I: Metals. J Biomed Mater Res B Appl Biomater 105:2162-2173
Gibon, Emmanuel; Córdova, Luis A; Lu, Laura et al. (2017) The biological response to orthopedic implants for joint replacement. II: Polyethylene, ceramics, PMMA, and the foreign body reaction. J Biomed Mater Res B Appl Biomater 105:1685-1691
Pajarinen, Jukka; Nabeshima, Akira; Lin, Tzu-Hua et al. (2017) * Murine Model of Progressive Orthopedic Wear Particle-Induced Chronic Inflammation and Osteolysis. Tissue Eng Part C Methods 23:1003-1011
Lin, T-H; Pajarinen, J; Lu, L et al. (2017) NF-?B as a Therapeutic Target in Inflammatory-Associated Bone Diseases. Adv Protein Chem Struct Biol 107:117-154
Lin, Tzu-Hua; Gibon, Emmanuel; Loi, Florence et al. (2017) Decreased osteogenesis in mesenchymal stem cells derived from the aged mouse is associated with enhanced NF-?B activity. J Orthop Res 35:281-288

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