Abstract

Orthopedic implants are the most common approach to repair degenerative and failing joints as well as segmental bone defects. However, inflammation and ensuing osteolysis are frequent complications of orthopedic implants arising in response to implant-derived debris. Subsequent revision surgeries are more challenging and carry greater risk of failure, morbidity and mortality, especially in the aging population. Our lon-term research goal is to decipher the biologic and pathologic mechanisms underlying implant debris- mediated osteolysis. In previous work, we have shown orthopedic particles (PMMA, PE, etc.) target osteoclast (OC) progenitors and activate NF-?B pathway, which is considered central for inflammatory responses and essential for OC differentiation. We further showed that PMMA particles enhance NF-?B activation by targeting TAK1, NEMO, TRAF6, and IKK2. This process exacerbates osteoclastogenesis and leads to osteolysis. Recently, we identified a novel mechanism underlying regulation of TRAF6/NEMO/IKK2 signaling complex by the forkhead protein Foxp3 in regulatory T cells (Tregs), leading to NF-?B activation, abundant production of growth factors, cytokines and chemokine. This hyper-cytokinemia led to hyperproliferation of hematopoietic stem cells (HSCs) and to expansion of early/primitive population of myeloid progenitors that possessed high OC potential. We now have evidence that PMMA particles induce this inflammatory pathway, in vivo. We also found that PMMA particles directly regulate Notch/RNBPJ signaling in myeloid progenitors leading to activation of OC-related transcription factors (NF-?B and NFATc1). Hence, we posit that PMMA particles, and likely other implant materials, trigger inflammatory paracrinic and autocrinic signaling circuits in multiple cell typesin the bone marrow microenvironment including lymphocytes and myeloid progenitors. The signaling switches of these circuits include Foxp3, Notch/RBPJ, and NF-?B transcription factors, driving myeloid cell expansion in response to bone marrow stress in paracrinic and autocrinic modes. Based on this information, we hypothesize that PMMA particles, by unidentified stress mechanism, modulate T cell activation by down-regulating Foxp3 function, resulting with T cell phenotypic switch into pathogenic T helper cells with enhanced NF-?B activity. This step leads to production of osteotropic and pro-inflammatory factors that expand the myelo-progenitor population and enhance OC formation. We further hypothesize that PMMA particles contribute to activation of Notch signaling directly in myeloid progenitors leading to activation of RBPJ and NFATc1. Hence we propose to: 1) Investigate the paracrine mechanism(s) by which PMMA particles target lymphocytes to enhance myelo- proliferation and increase OC burden, 2) Investigate the autocrine mechanism underlying PMMA regulation of myelo-proliferation in OCPs by RBPJ and its contribution to osteoclastogenesis, and 3) Determine the role of Foxp3 and RBPJ in PMMA-induced tibial and calvarial osteolysis. Appropriate cellular, molecular, and genetic mouse models and tools will be used to test these Aims.

Public Health Relevance

Inflammatory osteolysis is a major complication of orthopedic joint implants. Debris released from these implants trigger immune and inflammatory responses that generate ideal conditions for recruitment of bone resorbing cells to the injury site. The ensuing pathologic bone erosion around the implant leads to loosening and ultimately failure of implants. The health costs for revision surgeries are high and pose a great burden on the health care system. More importantly, morbidity and mortality associated with this disease are high. Although great progress related to material quality and technical aspects of implant surgery have been made, the details of the biologic response to implant debris remain enigmatic. Our study offers a promising approach to define the mechanism by which PMMA particles modulate immune cell phenotype and function, and subsequently alter myeloid lineage frequency and osteoclastogenic potential. The combination of these effects exacerbates osteoclasts and osteolysis. We are confident that the results of our research will decipher the cellular response to particles and will eventually benefit management (treatment and prevention) of inflammatory osteolysis to great extent.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR049192-12
Application #
9103865
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Washabaugh, Charles H
Project Start
2002-12-01
Project End
2020-06-30
Budget Start
2016-07-01
Budget End
2017-06-30
Support Year
12
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Orthopedics
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Wang, Chun; Hockerman, Susan; Jacobsen, E Jon et al. (2018) Selective inhibition of the p38? MAPK-MK2 axis inhibits inflammatory cues including inflammasome priming signals. J Exp Med 215:1315-1325
Wang, Cuicui; Abu-Amer, Yousef; O'Keefe, Regis J et al. (2018) Loss of Dnmt3b in Chondrocytes Leads to Delayed Endochondral Ossification and Fracture Repair. J Bone Miner Res 33:283-297
Wang, Chun; Xu, Can-Xin; Alippe, Yael et al. (2017) Chronic inflammation triggered by the NLRP3 inflammasome in myeloid cells promotes growth plate dysplasia by mesenchymal cells. Sci Rep 7:4880
Alippe, Yael; Wang, Chun; Ricci, Biancamaria et al. (2017) Bone matrix components activate the NLRP3 inflammasome and promote osteoclast differentiation. Sci Rep 7:6630
Swarnkar, Gaurav; Chen, Tim Hung-Po; Arra, Manoj et al. (2017) NUMBL Interacts with TAK1, TRAF6 and NEMO to Negatively Regulate NF-?B Signaling During Osteoclastogenesis. Sci Rep 7:12600
Zou, Wei; Rohatgi, Nidhi; Chen, Timothy Hung-Po et al. (2016) PPAR-? regulates pharmacological but not physiological or pathological osteoclast formation. Nat Med 22:1203-1205
Wang, C; Qu, C; Alippe, Y et al. (2016) Poly-ADP-ribosylation-mediated degradation of ARTD1 by the NLRP3 inflammasome is a prerequisite for osteoclast maturation. Cell Death Dis 7:e2153
Swarnkar, Gaurav; Shim, Kyuhwan; Nasir, Amjad M et al. (2016) Myeloid Deletion of Nemo Causes Osteopetrosis in Mice Owing to Upregulation of Transcriptional Repressors. Sci Rep 6:29896
Swarnkar, Gaurav; Karuppaiah, Kannan; Mbalaviele, Gabriel et al. (2015) Osteopetrosis in TAK1-deficient mice owing to defective NF-?B and NOTCH signaling. Proc Natl Acad Sci U S A 112:154-9
Swarnkar, Gaurav; Abu-Amer, Yousef (2015) Regulation of NF-?B signaling in osteoclasts and myeloid progenitors. Methods Mol Biol 1280:527-42

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