论文信息 - Macrophages-Key cells in the response to wear debris from joint replacements.

Macrophages-Key cells in the response to wear debris from joint replacements.

The generation of wear debris is an inevitable result of normal usage of joint replacements. Wear debris particles stimulate local and systemic biological reactions resulting in chronic inflammation, periprosthetic bone destruction, and eventually, implant loosening, and revision surgery. The latter may be indicated in up to 15% patients in the decade following the arthroplasty using conventional polyethylene. Macrophages play multiple roles in both inflammation and in maintaining tissue homeostasis. As sentinels of the innate immune system, they are central to the initiation of this inflammatory cascade, characterized by the release of proinflammatory and pro-osteoclastic factors. Similar to the response to pathogens, wear particles elicit a macrophage response, based on the unique properties of the cells belonging to this lineage, including sensing, chemotaxis, phagocytosis, and adaptive stimulation. The biological processes involved are complex, redundant, both local and systemic, and highly adaptive. Cells of the monocyte/macrophage lineage are implicated in this phenomenon, ultimately resulting in differentiation and activation of bone resorbing osteoclasts. Simultaneously, other distinct macrophage populations inhibit inflammation and protect the bone-implant interface from osteolysis. Here, the current knowledge about the physiology of monocyte/macrophage lineage cells is reviewed. In addition, the pattern and consequences of their interaction with wear debris and the recent developments in this field are presented.

[1] J. Fisher,et al. Effect of size and dose on bone resorption activity of macrophages by in vitro clinically relevant ultra high molecular weight polyethylene particles. , 2000, Journal of biomedical materials research.

[2] B. Morrey,et al. Twenty-five-Year Survivorship of Two Thousand Consecutive Primary Charnley Total Hip Replacements: Factors Affecting Survivorship of Acetabular and Femoral Components , 2002, The Journal of bone and joint surgery. American volume.

[3] Steffen Jung,et al. Distinct Differentiation Potential of Blood Monocyte Subsets in the Lung1 , 2007, The Journal of Immunology.

[4] S. Goodman. Wear particles, periprosthetic osteolysis and the immune system. , 2007, Biomaterials.

[5] J. Edwards,et al. Exploring the full spectrum of macrophage activation , 2008, Nature Reviews Immunology.

[6] J. Babensee,et al. Macrophage and dendritic cell phenotypic diversity in the context of biomaterials. , 2011, Journal of biomedical materials research. Part A.

[7] J. Charnley,et al. The long-term results of low-friction arthroplasty of the hip performed as a primary intervention. , 1972, The Journal of bone and joint surgery. British volume.

[8] Edward Ebramzadeh,et al. Histological Features of Pseudotumor-like Tissues From Metal-on-Metal Hips , 2010, Clinical orthopaedics and related research.

[9] S. Goodman,et al. Effects of orthopedic polymer particles on chemotaxis of macrophages and mesenchymal stem cells. , 2010, Journal of biomedical materials research. Part A.

[10] M. Smeltzer,et al. Is aseptic loosening truly aseptic? , 2005, Clinical orthopaedics and related research.

[11] Hideo Negishi,et al. Regulation of innate immune responses by DAI (DLM-1/ZBP1) and other DNA-sensing molecules , 2008, Proceedings of the National Academy of Sciences.

[12] T. Bauer,et al. Characterization and Comparison of Wear Debris from Failed Total Hip Implants of Different Types* , 1996, The Journal of bone and joint surgery. American volume.

[13] J. Greenleaf,et al. Sonication of removed hip and knee prostheses for diagnosis of infection. , 2007, The New England journal of medicine.

[14] S. Badylak,et al. Macrophage participation in the degradation and remodeling of extracellular matrix scaffolds. , 2009, Tissue engineering. Part A.

[15] S. Gordon. Alternative activation of macrophages , 2003, Nature Reviews Immunology.

[16] Markus G. Manz,et al. Development of Monocytes, Macrophages, and Dendritic Cells , 2010, Science.

[17] S. Akira,et al. Toll-like receptors in innate immunity. , 2004, International immunology.

[18] L. Santambrogio,et al. Mediators of the inflammatory response to joint replacement devices , 2011, Nature Reviews Rheumatology.

[19] B. Wroblewski,et al. Long‐term Results of Low‐friction Arthroplasty in Patients 30 Years of Age or Younger , 1986, Clinical orthopaedics and related research.

[20] H. Rubash,et al. Human macrophage response to UHMWPE, TiAlV, CoCr, and alumina particles: analysis of multiple cytokines using protein arrays. , 2008, Journal of biomedical materials research. Part A.

[21] T. Hohl,et al. Monocyte-mediated defense against microbial pathogens. , 2008, Annual review of immunology.

[22] L. Bai,et al. Polymethylmethacrylate and titanium alloy particles activate peripheral monocytes during periprosthetic inflammation and osteolysis , 2011, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[23] W. Maloney,et al. Induction of macrophage C-C chemokine expression by titanium alloy and bone cement particles , 1999 .

[24] S. Goodman,et al. Revision joint replacement, wear particles, and macrophage polarization. , 2012, Acta biomaterialia.

[25] R. Steinman,et al. Dendritic cell progenitors phagocytose particulates, including bacillus Calmette-Guerin organisms, and sensitize mice to mycobacterial antigens in vivo , 1993, The Journal of experimental medicine.

[26] S. Amini,et al. Monocyte chemoattractant protein-1 (MCP-1): an overview. , 2009, Journal of interferon & cytokine research : the official journal of the International Society for Interferon and Cytokine Research.

[27] S. Goodman,et al. Surveillance of systemic trafficking of macrophages induced by UHMWPE particles in nude mice by noninvasive imaging. , 2010, Journal of biomedical materials research. Part A.

[28] S. Goodman,et al. Continuous Infusion of UHMWPE Particles Induces Increased Bone Macrophages and Osteolysis , 2011, Clinical orthopaedics and related research.

[29] C. Dinarello. A clinical perspective of IL‐1β as the gatekeeper of inflammation , 2011, European journal of immunology.

[30] S. Goodman,et al. Systemic trafficking of macrophages induced by bone cement particles in nude mice. , 2008, Biomaterials.

[31] Shizuo Akira,et al. Innate immune recognition of viral infection , 2006, Nature Immunology.

[32] S. Akira,et al. Toll-like receptors: critical proteins linking innate and acquired immunity , 2001, Nature Immunology.

[33] S Gordon,et al. Interleukin 4 potently enhances murine macrophage mannose receptor activity: a marker of alternative immunologic macrophage activation , 1992, The Journal of experimental medicine.

[34] James M. Anderson,et al. Foreign body reaction to biomaterials. , 2008, Seminars in immunology.

[35] C. Lowell,et al. Integrin signalling in neutrophils and macrophages. , 1999, Cellular signalling.

[36] L. Santambrogio,et al. Immunogenecity of Modified Alkane Polymers Is Mediated through TLR1/2 Activation , 2008, PloS one.

[37] E. Schwarz,et al. Periprosthetic osteolysis: an immunologist's update , 2006, Current opinion in rheumatology.

[38] B. Espehaug,et al. Patient-related risk factors for early revision of total hip replacements. A population register-based case-control study of 674 revised hips. , 1997, Acta orthopaedica Scandinavica.

[39] R. Steinman,et al. Differentiation of monocytes into dendritic cells in a model of transendothelial trafficking. , 1998, Science.

[40] C. Engh,et al. Osteolysis propensity among bilateral total hip arthroplasty patients. , 2011, The Journal of arthroplasty.

[41] V. Denaro,et al. Genetic susceptibility to aseptic loosening following total hip arthroplasty: a systematic review. , 2012, British medical bulletin.

[42] C. R. Howlett,et al. Macrophages at the skeletal tissue-device interface of loosened prosthetic devices express bone-related genes and their products. , 2003, Journal of biomedical materials research. Part A.

[43] Y. Konttinen,et al. Increased Expression of Toll-like Receptors in Aseptic Loose Periprosthetic Tissues and Septic Synovial Membranes Around Total Hip Implants , 2009, The Journal of Rheumatology.

[44] R. Creusot. NF-κB in DCs: it takes effort to be immature , 2011, Nature Medicine.

[45] H. Rubash,et al. Assessing osteolysis with use of high-throughput protein chips. , 2007, The Journal of bone and joint surgery. American volume.

[46] T. Kodama,et al. Defective Microarchitecture of the Spleen Marginal Zone and Impaired Response to a Thymus-Independent Type 2 Antigen in Mice Lacking Scavenger Receptors MARCO and SR-A1 , 2005, The Journal of Immunology.

[47] J. Casanova,et al. Human CD14dim Monocytes Patrol and Sense Nucleic Acids and Viruses via TLR7 and TLR8 Receptors , 2010, Immunity.

[48] J. Dick,et al. Revised map of the human progenitor hierarchy shows the origin of macrophages and dendritic cells in early lymphoid development , 2010, Nature Immunology.

[49] L. Joosten,et al. IL-17 Promotes Bone Erosion in Murine Collagen-Induced Arthritis Through Loss of the Receptor Activator of NF-κB Ligand/Osteoprotegerin Balance 1 , 2003, The Journal of Immunology.

[50] R. Barrack,et al. Improved cementing techniques and femoral component loosening in young patients with hip arthroplasty. A 12-year radiographic review. , 1992, The Journal of bone and joint surgery. British volume.

[51] J. Moreland,et al. Wear Is a Function of Use, Not Time , 2000, Clinical orthopaedics and related research.

[52] G Shimamoto,et al. Osteoprotegerin: A Novel Secreted Protein Involved in the Regulation of Bone Density , 1997, Cell.

[53] S. Santavirta,et al. The microenvironment around total hip replacement prostheses. , 2005, Clinical orthopaedics and related research.

[54] K. Schäkel,et al. The CD16+ (FcγRIII+) Subset of Human Monocytes Preferentially Becomes Migratory Dendritic Cells in a Model Tissue Setting , 2002, The Journal of experimental medicine.

[55] W. Maloney,et al. Cellular profile and cytokine production at prosthetic interfaces: Study of tissues retrieved from revised hip and knee replacements , 1998 .

[56] R E Booth,et al. Survivorship analysis of 1,041 Charnley total hip arthroplasties. , 1990, The Journal of arthroplasty.

[57] N. Morrison,et al. Induction of chemokines and chemokine receptors CCR2b and CCR4 in authentic human osteoclasts differentiated with RANKL and osteoclast like cells differentiated by MCP‐1 and RANTES , 2006, Journal of cellular biochemistry.

[58] P. Hoffmeyer,et al. Influence of patient activity on femoral osteolysis at five and ten years following hybrid total hip replacement. , 2011, The Journal of bone and joint surgery. British volume.

[59] S. Goodman,et al. The relationship of polyethylene wear to particle size, distribution, and number: A possible factor explaining the risk of osteolysis after hip arthroplasty. , 2010, Journal of biomedical materials research. Part B, Applied biomaterials.

[60] B. Christensen,et al. C-terminal Modification of Osteopontin Inhibits Interaction with the αVβ3-Integrin* , 2011, The Journal of Biological Chemistry.

[61] D. Graves,et al. Monocyte chemoattractant protein-1 regulates adhesion molecule expression and cytokine production in human monocytes. , 1992, Journal of immunology.

[62] Silvano Sozzani,et al. The chemokine system in diverse forms of macrophage activation and polarization. , 2004, Trends in immunology.

[63] H. Amstutz,et al. The pathology of failed total joint arthroplasty. , 1982, Clinical orthopaedics and related research.

[64] Y. Konttinen,et al. Toll-like receptors in the interface membrane around loosening total hip replacement implants. , 2007, Journal of biomedical materials research. Part A.

[65] L. Santambrogio,et al. Endosomal damage and TLR2 mediated inflammasome activation by alkane particles in the generation of aseptic osteolysis. , 2009, Molecular immunology.

[66] Y. Konttinen,et al. Enhanced osteolytic potential of monocytes/macrophages derived from bone marrow after particle stimulation. , 2008, Journal of biomedical materials research. Part B, Applied biomaterials.

[67] Sandra L. Schmid,et al. Regulated portals of entry into the cell , 2003, Nature.

[68] L. Lum,et al. Evidence for a Role of a Tumor Necrosis Factor-α (TNF-α)-converting Enzyme-like Protease in Shedding of TRANCE, a TNF Family Member Involved in Osteoclastogenesis and Dendritic Cell Survival* , 1999, Journal of Biological Chemistry.

[69] D. Macdonald,et al. Variation in the TNF Gene Promoter and Risk of Osteolysis After Total Hip Arthroplasty , 2003, Journal of bone and mineral research : the official journal of the American Society for Bone and Mineral Research.

[70] J. Suttles,et al. Macrophages Sequentially Change Their Functional Phenotype in Response to Changes in Microenvironmental Influences1 , 2005, The Journal of Immunology.

[71] R. Schwendener,et al. Macrophage depletion diminishes implant-wear-induced inflammatory osteolysis in a mouse model. , 2008, Journal of biomedical materials research. Part A.

[72] S. Reuter,et al. DC-derived IL-18 drives Treg differentiation, murine Helicobacter pylori-specific immune tolerance, and asthma protection. , 2012, The Journal of clinical investigation.

[73] Mark Baer,et al. Tumor Necrosis Factor Alpha Transcription in Macrophages Is Attenuated by an Autocrine Factor That Preferentially Induces NF-κB p50 , 1998, Molecular and Cellular Biology.

[74] L. Kobzik,et al. Disparate Regulation and Function of the Class A Scavenger Receptors SR-AI/II and MARCO1 , 2005, The Journal of Immunology.

[75] T. Uede. Osteopontin, intrinsic tissue regulator of intractable inflammatory diseases , 2011, Pathology international.

[76] W H Harris,et al. Formation of a synovial-like membrane at the bone-cement interface. Its role in bone resorption and implant loosening after total hip replacement. , 1986, Arthritis and rheumatism.

[77] D. Klee,et al. Topographical control of human macrophages by a regularly microstructured polyvinylidene fluoride surface. , 2008, Biomaterials.

[78] R. Eastell,et al. Variation in the secreted frizzled‐related protein‐3 gene and risk of Osteolysis and heterotopic ossification after total hip arthroplasty , 2007, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[79] A. Marshak‐Rothstein,et al. Toll‐like receptors, endogenous ligands, and systemic autoimmune disease , 2005, Immunological reviews.

[80] Y. Konttinen,et al. Toll‐like receptors and their adaptors are regulated in macrophages after phagocytosis of lipopolysaccharide‐coated titanium particles , 2011, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[81] H. Nückel,et al. BCL2-938C > A and CALCA-1786T > C polymorphisms in aseptic loosened total hip arthroplasty , 2009, European journal of medical research.

[82] Victor M. Goldberg,et al. Bacterial Pathogen-associated Molecular Patterns Stimulate Biological Activity of Orthopaedic Wear Particles by Activating Cognate Toll-like Receptors* , 2010, The Journal of Biological Chemistry.

[83] R. Medzhitov. Origin and physiological roles of inflammation , 2008, Nature.

[84] S. Akira,et al. Species-Specific Recognition of Single-Stranded RNA via Toll-like Receptor 7 and 8 , 2004, Science.

[85] J. Older. Charnley low-friction arthroplasty: a worldwide retrospective review at 15 to 20 years. , 2002, The Journal of arthroplasty.

[86] B. Rollins,et al. The effect of MCP-1 depletion on chemokine and chemokine-related gene expression: evidence for a complex network in acute inflammation. , 2005, Cytokine.

[87] D. Lindsey,et al. An in vivo murine model of continuous intramedullary infusion of polyethylene particles. , 2008, Biomaterials.

[88] Liping Tang,et al. Molecular determinants of biocompatibility , 2005, Expert review of medical devices.

[89] John Fisher,et al. The role of macrophages in osteolysis of total joint replacement. , 2005, Biomaterials.

[90] T. Martin,et al. Tumor Necrosis Factor (cid:97) Stimulates Osteoclast Differentiation by a Mechanism Independent of the ODF/RANKL–RANK Interaction , 2022 .

[91] M. Gale,et al. Immune signaling by RIG-I-like receptors. , 2011, Immunity.

[92] A Sarmiento,et al. The origin of submicron polyethylene wear debris in total hip arthroplasty. , 1995, Clinical orthopaedics and related research.

[93] S. Santavirta,et al. Acid Attack and Cathepsin K in Bone Resorption Around Total Hip Replacement Prosthesis , 2001, Journal of bone and mineral research : the official journal of the American Society for Bone and Mineral Research.

[94] S. Akira,et al. The innate immune response to bacterial flagellin is mediated by Toll-like receptor 5 , 2001, Nature.

[95] M. Hickey,et al. Mechanisms of Disease: macrophage migration inhibitory factor in SLE, RA and atherosclerosis , 2008, Nature Clinical Practice Rheumatology.

[96] J. Jacobs,et al. Soluble and particulate Co‐Cr‐Mo alloy implant metals activate the inflammasome danger signaling pathway in human macrophages: A novel mechanism for implant debris reactivity , 2009, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[97] F. Osorio,et al. Myeloid C-type lectin receptors in pathogen recognition and host defense. , 2011, Immunity.

[98] J. Callaghan,et al. Charnley Total Hip Arthroplasty in Patients Less Than Fifty Years Old. A Twenty to Twenty-five-Year Follow-up Note* , 1998, The Journal of bone and joint surgery. American volume.

[99] V. Goldberg,et al. Does endotoxin contribute to aseptic loosening of orthopedic implants? , 2005, Journal of biomedical materials research. Part B, Applied biomaterials.

[100] S. Gambhir,et al. Exogenous MC3T3 preosteoblasts migrate systemically and mitigate the adverse effects of wear particles. , 2012, Tissue engineering. Part A.

[101] S. Gordon,et al. Alternative activation of macrophages: an immunologic functional perspective. , 2009, Annual review of immunology.

[102] M. Takagi. Toll-like Receptor , 2011 .

[103] B. Wroblewski,et al. Charnley low-frictional torque arthroplasty: follow-up for 30 to 40 years. , 2009, The Journal of bone and joint surgery. British volume.

[104] G. Rodan,et al. Interleukin 1 induces multinucleation and bone-resorbing activity of osteoclasts in the absence of osteoblasts/stromal cells. , 1999, Experimental cell research.

[105] R. Flavell,et al. Recognition of double-stranded RNA and activation of NF-κB by Toll-like receptor 3 , 2001, Nature.

[106] Paul T. H. Lee,et al. Polymerase Chain Reaction Can Detect Bacterial DNA in Aseptically Loose Total Hip Arthroplasties , 2004, Clinical orthopaedics and related research.

[107] V. Goldberg,et al. Adherent endotoxin mediates biological responses of titanium particles without stimulating their phagocytosis , 2002, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[108] W. Robinson,et al. Role of the Toll-like receptor pathway in the recognition of orthopedic implant wear-debris particles. , 2011, Biomaterials.

[109] V. Goldberg,et al. Adherent Endotoxin on Orthopedic Wear Particles Stimulates Cytokine Production and Osteoclast Differentiation , 2001, Journal of bone and mineral research : the official journal of the American Society for Bone and Mineral Research.

[110] U. Frey,et al. Gender‐dependent association of the GNAS1 T393C polymorphism with early aseptic loosening after total hip arthroplasty , 2008, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[111] E. Greenfield,et al. Titanium particles activate toll‐like receptor 4 independently of lipid rafts in RAW264.7 murine macrophages , 2011, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[112] A. Cumano,et al. Monitoring of Blood Vessels and Tissues by a Population of Monocytes with Patrolling Behavior , 2007, Science.

[113] C. Figdor,et al. Toll-like receptor expression and function in human dendritic cell subsets: implications for dendritic cell-based anti-cancer immunotherapy , 2010, Cancer Immunology, Immunotherapy.

[114] A. Sica,et al. Macrophage polarization comes of age. , 2005, Immunity.

[115] L. Sly,et al. Generation and characterization of murine alternatively activated macrophages. , 2013, Methods in molecular biology.

[116] K Yano,et al. Osteoclast differentiation factor is a ligand for osteoprotegerin/osteoclastogenesis-inhibitory factor and is identical to TRANCE/RANKL. , 1998, Proceedings of the National Academy of Sciences of the United States of America.

[117] C. Lohmann,et al. Metal-on-metal bearings and hypersensitivity in patients with artificial hip joints. A clinical and histomorphological study. , 2005, The Journal of bone and joint surgery. American volume.

[118] K. Hasty,et al. Accumulation of LPS by polyethylene particles decreases bone attachment to implants , 2006, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[119] E. Gómez-Barrena,et al. Profile of toll-like receptor-positive cells in septic and aseptic loosening of total hip arthroplasty implants. , 2010, Journal of biomedical materials research. Part A.

[120] F. Geissmann,et al. Blood monocytes: development, heterogeneity, and relationship with dendritic cells. , 2009, Annual review of immunology.

[121] T. Muneta,et al. Osteopontin deficiency impairs wear debris-induced osteolysis via regulation of cytokine secretion from murine macrophages. , 2010, Arthritis and rheumatism.

[122] R. Caspi,et al. Th1 and Th17 cells , 2010, Annals of the New York Academy of Sciences.

[123] P. E. Purdue. Alternative macrophage activation in periprosthetic osteolysis , 2008, Autoimmunity.

[124] T. Bauer,et al. Isolation and characterization of debris in membranes around total joint prostheses. , 1994, The Journal of bone and joint surgery. American volume.

[125] M. Haniffa,et al. Human dendritic cell deficiency: the missing ID? , 2011, Nature Reviews Immunology.

[126] P. Allavena,et al. Infiltration of tumours by macrophages and dendritic cells: tumour-associated macrophages as a paradigm for polarized M2 mononuclear phagocytes. , 2004, Novartis Foundation symposium.

[127] L. Hofbauer,et al. Clinical implications of the osteoprotegerin/RANKL/RANK system for bone and vascular diseases. , 2004, JAMA.

[128] Y. Iwakura,et al. Periprosthetic osteolysis: Characterizing the innate immune response to titanium wear‐particles , 2010, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[129] E. Pamer,et al. Monocyte recruitment during infection and inflammation , 2011, Nature Reviews Immunology.

[130] Y. Konttinen,et al. Toll‐like receptors and aseptic loosening of hip endoprosthesis—a potential to respond against danger signals? , 2010, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[131] Y. Konttinen,et al. Biocompatibility of total joint replacements: A review. , 2009, Journal of biomedical materials research. Part A.

[132] R. Steinman,et al. High Levels of a Major Histocompatibility Complex II–Self Peptide Complex on Dendritic Cells from the T Cell Areas of Lymph Nodes , 1997, The Journal of experimental medicine.

[133] C. Selinger,et al. MCP-1-induced Human Osteoclast-like Cells Are Tartrate-resistant Acid Phosphatase, NFATc1, and Calcitonin Receptor-positive but Require Receptor Activator of NFκB Ligand for Bone Resorption* , 2006, Journal of Biological Chemistry.

[134] A. Sher,et al. Cooperation of Toll-like receptor signals in innate immune defence , 2007, Nature Reviews Immunology.

[135] J. Anderson,et al. Adsorbed IgG: a potent adhesive substrate for human macrophages. , 2000, Journal of biomedical materials research.

[136] J. Fisher,et al. A novel method for the prediction of functional biological activity of polyethylene wear debris , 2001, Proceedings of the Institution of Mechanical Engineers. Part H, Journal of engineering in medicine.

[137] S. Santavirta,et al. Interface tissue fibroblasts from loose total hip replacement prosthesis produce receptor activator of nuclear factor-kappaB ligand, osteoprotegerin, and cathepsin K. , 2005, The Journal of rheumatology.

[138] P. Campbell,et al. Isolation of predominantly submicron-sized UHMWPE wear particles from periprosthetic tissues. , 1995, Journal of biomedical materials research.

[139] N. E. Miller,et al. Regulation of macrophage activation , 2003, Cellular and Molecular Life Sciences CMLS.

[140] N. Udagawa,et al. Macrophage colony-stimulating factor is indispensable for both proliferation and differentiation of osteoclast progenitors. , 1993, The Journal of clinical investigation.

[141] D. W. Roberts,et al. Factors Influencing Wear and Osteolysis in Press-Fit Condylar Modular Total Knee Replacements , 2004, Clinical orthopaedics and related research.

[142] M. Selenius,et al. Ectopic expression of macrophage scavenger receptor MARCO in synovial membrane-like interface tissue in aseptic loosening of total hip replacement implants. , 2009, Journal of biomedical materials research. Part A.

[143] S. Goodman,et al. Selective inhibition of the MCP‐1‐CCR2 ligand‐receptor axis decreases systemic trafficking of macrophages in the presence of UHMWPE particles , 2012, Journal of orthopaedic research : official publication of the Orthopaedic Research Society.

[144] Michael J. Lee,et al. Lipopolysaccharide Found in Aseptic Loosening of Patients with Inflammatory Arthritis , 2006, Clinical orthopaedics and related research.