Acute transient inflammation is crucial for initiation of bone healing, osseointegration of implants, osteogenic differentiation of MSCs, and immunomodulation. However, harmful chronic inflammation and bone loss (osteolysis) are induced by adverse stimuli including wear byproducts from joint replacements (JR). Nuclear Factor kappa B (NF-?B) is a critical transcription factor in both macrophages (m?) and MSCs that regulates inflammation, bone formation/remodeling, and aging. We showed that preconditioning MSCs with lipopoly- saccharide (LPS) and tumor necrosis factor-? (TNF-?) to induce acute transient activation of NF-?B synergistically enhances osteogenesis, and modulates m? polarization from a pro-inflammatory (M1) to an anti-inflammatory pro-regenerative (M2) phenotype. Furthermore, inhibition of persistent NF-?B signaling using an NF-?B decoy OligoDeoxyNucleotide (ODN) was shown to mitigate inflammatory bone loss. We have genetically modified MSCs to sense NF-?B activation and then increase production of the anti-inflammatory pro-regenerative cytokine IL-4. The purpose of this grant is to accelerate net bone formation and mitigate chronic inflammation and osteolysis via NF-kB driven immunomodulation using preconditioned or genetically modified MSCs transplanted to the local environment.
Specific Aim #1 a -To define the critical immunomodulatory interactions of preconditioned vs. NF-?B sensing and IL-4 secreting MSCs on m? exposed to wear byproducts from orthopaedic implants.
Specific Aim #1 b - To enhance osteogenesis by using preconditioned vs. NF-?B sensing and IL-4 secreting MSCs in an MSC/m? co-culture model exposed to wear byproducts from orthopaedic implants.
Specific Aim #2 a - To demonstrate the therapeutic effects of transplanted preconditioned MSCs on bone during the acute inflammatory stage (simulating the stage of initial implantation of a prosthesis and osseointegration) using the murine continuous femoral particle infusion model.
Specific Aim #2 b - To demonstrate the therapeutic effects of preconditioned vs. NF-?B sensing and IL-4 secreting MSCs on net bone formation during the chronic inflammatory stage (simulating established wear particle disease) using the murine continuous femoral particle infusion model.
Specific Aim #3 - To demonstrate that the above principles of modulating acute and chronic inflammation are valid irrespective of animal sex (male vs. female mice) or age (young vs. elderly mice) in vivo. We hypothesize that NF-?B preconditioning or NF-?B sensing and IL-4 secreting MSCs will enhance the osteogenic and immunomodulatory signaling of MSCs, enhancing bone formation via crosstalk by m? and MSCs. NF-kB driven immunomodulation of MSCs should mitigate particle-induced inflammation, osteoclast activation, and enhance bone formation in young and aged, male and female mice. NF-kB driven immune modulation of MSCs is novel, mechanistic, and directly translational to inflammatory disorders in other organ systems.

Public Health Relevance

Acute transient inflammation is crucial for bone healing, integration of implants, differentiation of bone progenitor cells (MSCs), and immune modulation. However, wear byproducts from joint replacements (JR) causes harmful chronic inflammation and subsequent bone loss (osteolysis). Nuclear Factor kappa B (NF-?B) is the critical transcription factor in both immune cells (macrophages - m?) and MSCs that regulates inflammation, bone healing, and aging. The purpose of this grant is to accelerate bone formation and mitigate chronic inflammation and osteolysis via NF-kB driven immune modulation using preconditioned or genetically modified MSCs transplanted to the local bone environment in young and aged, male and female mice.

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR063717-09
Application #
9979754
Study Section
Musculoskeletal Tissue Engineering Study Section (MTE)
Program Officer
Washabaugh, Charles H
Project Start
2012-09-15
Project End
2022-07-31
Budget Start
2020-08-01
Budget End
2021-07-31
Support Year
9
Fiscal Year
2020
Total Cost
Indirect Cost
Name
Stanford University
Department
Orthopedics
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305
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Córdova, Luis A; Loi, Florence; Lin, Tzu-Hua et al. (2017) CCL2, CCL5, and IGF-1 participate in the immunomodulation of osteogenesis during M1/M2 transition in vitro. J Biomed Mater Res A 105:3069-3076
Nabeshima, Akira; Pajarinen, Jukka; Lin, Tzu-Hua et al. (2017) Mutant CCL2 protein coating mitigates wear particle-induced bone loss in a murine continuous polyethylene infusion model. Biomaterials 117:1-9
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

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