Alternatively activated macrophages actively inhibit proliferation of peripheral blood lymphocytes and CD4<sup>+</sup> T cells <i>in vitro</i>

Schebesch, Christa; Kodelja, Vitam; Müller, C.; Hakij, N.; Bisson, S.; Orfanos, C.E.; Goerdt, Sergij

doi:10.1046/j.1365-2567.1997.00371.x

Cited by 114 publications

(87 citation statements)

References 63 publications

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“…M2 cells are considered to induce Th2 differentiation of CD4 ϩ T cells and cause Th1 tolerance (38,51,69). They may have potential roles in immune suppression (34,62). Loke et al (34) reported that the IL-4-induced alternatively activated macrophages reversibly inhibited T cell proliferation by a cell-to-cell contact mechanism, similar to the suppression we observed in tumor progressors.…”

Section: Discussionsupporting

confidence: 72%

Nitric Oxide-Independent CTL Suppression during Tumor Progression: Association with Arginase-Producing (M2) Myeloid Cells

Liu

Ginderachter

Brys

et al. 2003

The Journal of Immunology

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Most of the mice bearing a s.c. BW-Sp3 lymphoma tumor mount a CD8+ T cell-mediated response resulting in tumor regression. Nonetheless, tumor progression occurs in some of the recipients and is associated with CTL inactivity. We demonstrated that T cell-activating APC were induced in regressors whereas T cell suppressive myeloid cells predominated in the spleen of progressors. Indeed, in vitro depletion of either the adherent or the CD11b+ populations restored T cell cytotoxicity and proliferation in these mice. This CTL inhibition was cell-to-cell contact-dependent but not mediated by NO. However, the same progressor suppressive cells prevented the activity of in vitro-restimulated CTLs derived from regressors in a cell-to-cell contact and NO-dependent fashion. Thus, either the NO-dependent or -independent suppressive pathway prevailed, depending on the target CTL population. In addition, the suppressive population expressed a high arginase activity, suggesting an association of the suppressive phenotype with alternatively activated (M2) myeloid cells. However, the high arginase activity is not directly involved in the suppressive process. Our results provide new insights for myeloid cell-mediated CTL inhibition during cancer progression.

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Section: Discussionsupporting

confidence: 72%

Nitric Oxide-Independent CTL Suppression during Tumor Progression: Association with Arginase-Producing (M2) Myeloid Cells

Liu

Ginderachter

Brys

et al. 2003

The Journal of Immunology

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“…Functionally, they can induce tolerance and down-regulate inflammatory responses (28). In one report, IL-4-stimulated human macrophages inhibited mitogen-mediated proliferation of CD4 ϩ lymphocytes by an as yet unknown mechanism (29). Our experiments suggest a relationship between our myeloid suppressors and the alternatively activated macrophages, particularly in the case of MSC-2, which not only gains the suppressive phenotype in response to IL-4 (Figs.…”

Section: Discussionsupporting

confidence: 53%

Immortalized Myeloid Suppressor Cells Trigger Apoptosis in Antigen-Activated T Lymphocytes

Apolloni

Bronte

Mazzoni

et al. 2000

The Journal of Immunology

146

124

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We described a generalized suppression of CTL anamnestic responses that occurred in mice bearing large tumor nodules or immunized with powerful recombinant viral immunogens. Immune suppression entirely depended on GM-CSF-driven accumulation of CD11b+/Gr-1+ myeloid suppressor cells (MSC) in secondary lymphoid organs. To further investigate the nature and properties of MSC, we immortalized CD11b+/Gr-1+ cells isolated from the spleens of immunosuppressed mice, using a retrovirus encoding the v-myc and v-raf oncogenes. Immortalized cells expressed monocyte/macrophage markers (CD11b, F4/80, CD86, CD11c), but they differed from previously characterized macrophage lines in their capacities to inhibit T lymphocyte activation. Two MSC lines, MSC-1 and MSC-2, were selected based upon their abilities to inhibit Ag-specific proliferative and functional CTL responses. MSC-1 line was constitutively inhibitory, while suppressive functions of MSC-2 line were stimulated by exposure to the cytokine IL-4. Both MSC lines triggered the apoptotic cascade in Ag-activated T lymphocytes by a mechanism requiring cell-cell contact. Some well-known membrane molecules involved in the activation of apoptotic pathways (e.g., TNF-related apoptosis-inducing ligand, Fas ligand, TNF-α) were ruled out as candidate effectors for the suppression mechanism. The immortalized myeloid lines represent a novel, useful tool to shed light on the molecules involved in the differentiation of myeloid-related suppressors as well as in the inhibitory pathway they use to control T lymphocyte activation.

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“…I g is produced by T cells upon cue from I 12 and MHC displayed on the membrane of C. A inhibits production of I g by T cells (7). Including an I g decay term gives the following:…”

Section: Resultsmentioning

confidence: 99%

“…Martinez and colleagues also refer to these as M1 macrophages, characterizing them as having elevated expression of MHC-II, CD80, and CD86 costimulatory molecules and promoting TH1 differentiation and IFN-␥ production by T cells via the production of IL-12 (4). A different, more recently studied class of macrophages, is known as alternatively activated macrophages (AAM) (2,(5)(6)(7)(8). Also referred to as M2a macrophages, these macrophages have a phenotype resembling macrophages activated by Interleukin-4 (IL-4) or IL-13 and are characterized by the up-regulation of scavenger receptors and the mannose receptor.…”

mentioning

confidence: 99%

Modeling the immune rheostat of macrophages in the lung in response to infection

Day¹,

Friedman²,

Schlesinger

2009

Proc. Natl. Acad. Sci. U.S.A.

126

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In the lung, alternatively activated macrophages (AAM) form the first line of defense against microbial infection. Due to the highly regulated nature of AAM, the lung can be considered as an immunosuppressive organ for respiratory pathogens. However, as infection progresses in the lung, another population of macrophages, known as classically activated macrophages (CAM) enters; these cells are typically activated by IFN-␥. CAM are far more effective than AAM in clearing the microbial load, producing proinflammatory cytokines and antimicrobial defense mechanisms necessary to mount an adequate immune response. Here, we are concerned with determining the first time when the population of CAM becomes more dominant than the population of AAM. This proposed ''switching time'' is explored in the context of Mycobacterium tuberculosis (MTb) infection. We have developed a mathematical model that describes the interactions among cells, bacteria, and cytokines involved in the activation of both AAM and CAM. The model, based on a system of differential equations, represents a useful tool to analyze strategies for reducing the switching time, and to generate hypotheses for experimental testing.alternatively activated macrophages ͉ lung innate immunity ͉ mycobacteria tuberculosis

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Alternatively activated macrophages actively inhibit proliferation of peripheral blood lymphocytes and CD4⁺ T cells in vitro

Cited by 114 publications

References 63 publications

Nitric Oxide-Independent CTL Suppression during Tumor Progression: Association with Arginase-Producing (M2) Myeloid Cells

Nitric Oxide-Independent CTL Suppression during Tumor Progression: Association with Arginase-Producing (M2) Myeloid Cells

Immortalized Myeloid Suppressor Cells Trigger Apoptosis in Antigen-Activated T Lymphocytes

Modeling the immune rheostat of macrophages in the lung in response to infection

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Alternatively activated macrophages actively inhibit proliferation of peripheral blood lymphocytes and CD4+ T cells in vitro

Cited by 114 publications

References 63 publications

Nitric Oxide-Independent CTL Suppression during Tumor Progression: Association with Arginase-Producing (M2) Myeloid Cells

Nitric Oxide-Independent CTL Suppression during Tumor Progression: Association with Arginase-Producing (M2) Myeloid Cells

Immortalized Myeloid Suppressor Cells Trigger Apoptosis in Antigen-Activated T Lymphocytes

Modeling the immune rheostat of macrophages in the lung in response to infection

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Alternatively activated macrophages actively inhibit proliferation of peripheral blood lymphocytes and CD4⁺ T cells in vitro