CD14 cooperates with complement receptor 3 to mediate MyD88-independent phagocytosis of<i>Borrelia burgdorferi</i>

Hawley, Kelly L.; Olson, Chris M.; Iglesias-Pedraz, Juan Manuel; Navasa, Nicolás; Cervantes, Jorge; Caimano, Melissa J.; Izadi, Hooman; Ingalls, Robin R.; Pal, Utpal; Salazar, Juan C.; Radolf, Justin D.; Anguíta, Juan

doi:10.1073/pnas.1112078109

Cited by 70 publications

(92 citation statements)

References 39 publications

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“…BMDM are commonly used in Lyme disease research as a representative macrophage for investigating in vitro cellular responses to B. burgdorferi infection (26)(27)(28)(29). Following the culture and differentiation of BM precursors into BMDM in our laboratory, these cells appear to take on an uncommitted or M2 phenotype, as determined by flow cytometry expression of NOS2 or CD206 (Fig.…”

Section: Resultsmentioning

confidence: 99%

Macrophage Polarization during Murine Lyme Borreliosis

2015

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Infection of C3H mice with Borrelia burgdorferi, the causative agent of Lyme disease, reliably produces an infectious arthritis and carditis that peak around 3 weeks postinfection and then spontaneously resolve. Macrophage polarization has been suggested to drive inflammation, the clearance of bacteria, and tissue repair and resolution in a variety of infectious disease models. During Lyme disease it is clear that macrophages are capable of clearing Borrelia spirochetes and exhausted neutrophils; however, the role of macrophage phenotype in disease development or resolution has not been studied. Using classical (NOS2) and alternative (CD206) macrophage subset-specific markers, we determined the phenotype of F4/80 ؉ macrophages within the joints and heart throughout the infection time course. Within the joint, CD206؉ macrophages dominated throughout the course of infection, and NOS2؉ macrophage numbers became elevated only during the peak of inflammation. We also found dual NOS2 ؉ CD206 ؉ macrophages which increased during resolution. In contrast to findings for the ankle joints, numbers of NOS2 ؉ and CD206؉ macrophages in the heart were similar at the peak of inflammation. 5-Lipoxygenase-deficient (5-LOX ؊/؊ ) mice, which display a failure of Lyme arthritis resolution, recruited fewer F4/80 ؉ cells to the infected joints and heart, but macrophage subset populations were unchanged. These results highlight differences in the inflammatory infiltrates during Lyme arthritis and carditis and demonstrate the coexistence of multiple macrophage subsets within a single inflammatory site. Macrophages play a dynamic role in the immune system as both inflammatory and anti-inflammatory mediators. Their phenotype is highly flexible and dependent upon the cytokine stimulus of the microenvironment they infiltrate (1). They are routinely classified as proinflammatory and immunomodulatory (M1) or anti-inflammatory and remodeling (M2) macrophages, but their phenotype actually lies within a spectrum of inflammatory to anti-inflammatory polarization (2). The language within the field is currently being modified to ensure that the macrophages being studied have a clear phenotypic description, and we use the nomenclature recently suggested (3). Within the last 15 years, much work has been done to phenotypically characterize macrophage subsets. Identifying unique surface and intracellular markers, as well as understanding transcriptional regulation, has allowed the importance of specific macrophage phenotypes in infectious and autoimmune models to be uncovered.Classically activated M1 macrophages are proinflammatory cells capable of destroying pathogens, tumor cells, and various foreign compounds. Stimulation of undifferentiated macrophages with lipopolysaccharide (LPS) and gamma interferon (IFN-␥), or tumor necrosis factor alpha (TNF-␣), induces polarization to the M1 phenotype (4, 5). They can be recognized both in vitro and in vivo by the production of nitric oxide species (NOS), as well as other proinflammatory molecules, including ...

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Section: Resultsmentioning

confidence: 99%

Macrophage Polarization during Murine Lyme Borreliosis

2015

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“…We are currently delineating the underlying mechanism by which OspC affects phagocytosis by macrophage. In this regard, it is known that phagocytosis of B. burgdorferi by macrophages involves several phagocytic receptors (91)(92)(93) and pattern recognition receptors (28,94). One possibility is that OspC alters phagocytic receptor profiles upon contact with macrophages.…”

Section: Discussionmentioning

confidence: 99%

Outer Surface Protein OspC Is an Antiphagocytic Factor That Protects Borrelia burgdorferi from Phagocytosis by Macrophages

et al. 2015

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cOuter surface protein C (OspC) is one of the major lipoproteins expressed on the surface of Borrelia burgdorferi during tick feeding and the early phase of mammalian infection. OspC is required for B. burgdorferi to establish infection in both immunocompetent and SCID mice and has been proposed to facilitate evasion of innate immune defenses. However, the exact biological function of OspC remains elusive. In this study, we showed that the ospC-deficient spirochete could not establish infection in NOD-scid IL2r␥ null mice that lack B cells, T cells, NK cells, and lytic complement. The ospC mutant also could not establish infection in anti-Ly6G-treated SCID and C3H/HeN mice (depletion of neutrophils). However, depletion of mononuclear phagocytes at the skin site of inoculation in SCID and C3H/HeN mice allowed the ospC mutant to establish infection in vivo. In phagocyte-depleted mice, the ospC mutant was able to colonize the joints and triggered neutrophilia during dissemination. Furthermore, we found that phagocytosis of green fluorescent protein (GFP)-expressing ospC mutant spirochetes by murine peritoneal macrophages and human THP-1 macrophage-like cells, but not in PMN-HL60, was significantly higher than parental wild-type B. burgdorferi strains, suggesting that OspC has an antiphagocytic property. In addition, overproduction of OspC in spirochetes also decreased the uptake of spirochetes by murine peritoneal macrophages. Together, our findings provide evidence that mononuclear phagocytes play a key role in clearance of the ospC mutant and that OspC promotes spirochetes' evasion of macrophages during early Lyme borreliosis. L yme disease, the most prevalent vector-borne illness in the United States (1), is a multisystem inflammatory disorder caused by infection with the spirochete Borrelia burgdorferi (2, 3). This spirochete is maintained in nature through a complex enzootic cycle involving Ixodes ticks and various small-mammal hosts. Humans, as accidental hosts, become infected after B. burgdorferiinfected ticks feed on them (4). Spirochetes replicate in the skin, spread locally, and induce an inflammatory response with a symptom known as erythema migrans, observed in most patients (2, 4). During disseminated infection, B. burgdorferi colonizes multiple tissues, leading to different clinical manifestations, including arthritis, myocarditis, and neurological and/or cutaneous abnormalities (2, 4). This acute, disseminated stage of human Lyme disease is largely recapitulated using inbred mouse strains which are susceptible to B. burgdorferi infection and develop carditis and subacute arthritis (5). Thus, the murine model provides a powerful tool to elucidate the role of spirochete virulence factors and host immunological responses during Lyme disease pathogenesis (4).The B. burgdorferi genome encodes a large number of surface lipoproteins, many of which are expressed during mammalian infection (4, 6, 7). One of these lipoproteins is the major outer surface protein C (OspC), whose production is induced within inf...

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“…For example, macrophage activation via IFN-␥ or its suppression by IL-10 regulate their ability to phagocytose and destroy spirochetes (45)(46)(47). Importantly, the type of inflammatory cytokines elaborated by macrophages depends on the type of receptors engaged in the initial phagocytosis of B. burgdorferi (48), and this in turn likely is influenced by the activation stage of the macrophage, which itself is dependent on cytokines, such as IFN-␥, elaborated by CD4 T cells and iNKT cells (47). The outcome of these diverse effects of CD4 T cells on the control of Borrelia-induced disease appears strongly tissue dependent.…”

Section: Discussionmentioning

confidence: 99%

CD4⁺T Cells Promote Antibody Production but Not Sustained Affinity Maturation during Borrelia burgdorferi Infection

2015

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CD14 cooperates with complement receptor 3 to mediate MyD88-independent phagocytosis ofBorrelia burgdorferi

Cited by 70 publications

References 39 publications

Macrophage Polarization during Murine Lyme Borreliosis

Macrophage Polarization during Murine Lyme Borreliosis

Outer Surface Protein OspC Is an Antiphagocytic Factor That Protects Borrelia burgdorferi from Phagocytosis by Macrophages

CD4⁺T Cells Promote Antibody Production but Not Sustained Affinity Maturation during Borrelia burgdorferi Infection

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CD14 cooperates with complement receptor 3 to mediate MyD88-independent phagocytosis ofBorrelia burgdorferi

Cited by 70 publications

References 39 publications

Macrophage Polarization during Murine Lyme Borreliosis

Macrophage Polarization during Murine Lyme Borreliosis

Outer Surface Protein OspC Is an Antiphagocytic Factor That Protects Borrelia burgdorferi from Phagocytosis by Macrophages

CD4+T Cells Promote Antibody Production but Not Sustained Affinity Maturation during Borrelia burgdorferi Infection

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CD4⁺T Cells Promote Antibody Production but Not Sustained Affinity Maturation during Borrelia burgdorferi Infection