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...istochemica et Cytobiologica 2011, Vol. 49, No. 3, 365–374) Key words: CD163, inflammation Introduction Monocytes and macrophages play an important role in the regulation of the inflammatory response =-=[1, 2]-=-. Based on their functional properties, at least two subpopulations (M1 and M2) of mononuclear phagocytes, which differ in their pro- and anti-inflammatory potential, have been described [3]. The cell...

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...re divided according to their expression of the endotoxin receptor (CD14) and the high affinity immunoglobulin G receptor type III (FcgRIII — CD16), four different subpopulations can be distinguished =-=[18, 19]-=-. The highest expression of CD163 is found on CD14highCD16+ and the lowest on CD14lowCD16– cells [18, 19]. Cells in the CD14highCD16+ subpopulation have been reported to exert predominantly anti-infla...

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...h differentiation of such cells into macrophages [14–17]. Original reports using Ber-Mac3 or RM3/1 antibodies demonstrated expression of CD163 on 5% or 30% of freshly isolated monocytes, respectively =-=[14, 15]-=-. More recent reports, however, have demonstrated CD163 expression on a majority of peripheral blood monocytes [16, 17]. The discrepancies in reported expression of CD163 on freshly isolated periphera...

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... induced by CD4+CD25+Foxp3+ T regulatory cells and for rebound up-regulation of monocyte/macrophage CD163 expression after shedding of the receptor in response to Toll like receptor (TLR) stimulation =-=[27, 28]-=-. Glucocorticoids are at least equally potent inducers of CD163 expression [16, 26]. The magnitude of up-regulation of CD163 expression depends on the potency of the glucocorticoid: those having the g...

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...sponse [1, 2]. Based on their functional properties, at least two subpopulations (M1 and M2) of mononuclear phagocytes, which differ in their pro- and anti-inflammatory potential, have been described =-=[3]-=-. The cells of the M1 subpopulation secrete predominantly pro-inflammatory mediators which trigger and amplify inflammatory responses. Those of the M2 subpopulation produce mainly anti-inflammatory me...

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... CD163 binds to hemoglobin-haptoglobin (Hb-Hp) complexes, resulting in internalization of the complexes and preventing oxidative stress and inflammation associated with extracellular metabolism of Hb =-=[50]-=-. Using a ligand-affinity approach, CD163 was shown to be a specific receptor for Hb-Hp complexes, but not for Hb or Hp alone [50]. When released from erythrocytes, Hb binds to Hp to form complexes co...

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...ucocorticoids and interleukin-10 (IL-10) [16, 18, 23–26]. In fact, in experiments utilizing gene-chip technology, CD163 displays the strongest response to IL-10 among all 19 of the up-regulated genes =-=[25]-=-. Interleukin 10 is also responsible for up-regulation of monocyte/macrophage CD163 expression induced by CD4+CD25+Foxp3+ T regulatory cells and for rebound up-regulation of monocyte/macrophage CD163 ...

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...ot only does cell surface CD163 play a role in the modulation of the inflammatory response, soluble CD163 (sCD163) also can actively regulate that process. Soluble CD163 inhibits T cell proliferation =-=[63, 64]-=-. Purified sCD163 inhibited in a dose-dependent manner phorbol ester-induced T cell proliferation in vitro, at an optimal concentration of sCD163 of 0.5 mcg/ml [63, 64]. This anti-proliferatory functi...

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...h differentiation of such cells into macrophages [14–17]. Original reports using Ber-Mac3 or RM3/1 antibodies demonstrated expression of CD163 on 5% or 30% of freshly isolated monocytes, respectively =-=[14, 15]-=-. More recent reports, however, have demonstrated CD163 expression on a majority of peripheral blood monocytes [16, 17]. The discrepancies in reported expression of CD163 on freshly isolated periphera...

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...wever, CD163, in contrast to TLRs, can recognize and bind intact bacteria and not only soluble microbial components [56]. In pigs, an important role of CD163 in viral infections has been demonstrated =-=[57, 58]-=-. Two viruses, African swine fever virus (ASFV) and porcine reproductive and respiratory syndrome virus (PRRSV), use CD163 as an entry into the target cells of pigs [57, 58]. The ASFV uses CD163 as a ...

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... induced by CD4+CD25+Foxp3+ T regulatory cells and for rebound up-regulation of monocyte/macrophage CD163 expression after shedding of the receptor in response to Toll like receptor (TLR) stimulation =-=[27, 28]-=-. Glucocorticoids are at least equally potent inducers of CD163 expression [16, 26]. The magnitude of up-regulation of CD163 expression depends on the potency of the glucocorticoid: those having the g...

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...CD163. One of the anti-CD163 antibodies, Ki-m8, possesses agonistic properties, and it has been shown that application of this antibody leads to induction of IL-10 secretion by mononuclear phagocytes =-=[49]-=-. In 2001, Kristiansen et al. demonstrated that CD163 binds to hemoglobin-haptoglobin (Hb-Hp) complexes, resulting in internalization of the complexes and preventing oxidative stress and inflammation ...

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...3 [54]. TWEAK is a member of the TNF superfamily and plays many important roles in the processes associated with tissue damage and repair, e.g. inflammation, proliferation, apoptosis and angiogenesis =-=[59]-=-. Its ability to regulate innate and adaptive immune response seems to be one of the most interesting aspects of TWEAK from an immunological point of view [60]. In mice with genetically silenced TWEAK...

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...been shown to involve a metalloproteinase-dependent process [29, 32]. The same mechanism is responsible for down-regulation of monocyte CD163 expression by oxidative stress or 8-iso-prostaglandin F2a =-=[33]-=-. Prolonged stimulation with cell membrane TLR agonists, however, leads to a rebound up-regulation of CD163 to levels higher than those observed before stimulation with TLR ligands [28]. This effect d...

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...ot only does cell surface CD163 play a role in the modulation of the inflammatory response, soluble CD163 (sCD163) also can actively regulate that process. Soluble CD163 inhibits T cell proliferation =-=[63, 64]-=-. Purified sCD163 inhibited in a dose-dependent manner phorbol ester-induced T cell proliferation in vitro, at an optimal concentration of sCD163 of 0.5 mcg/ml [63, 64]. This anti-proliferatory functi...

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...alveolar macrophages [12, 20]. The level of expression of CD163 on tissue macrophages has been shown to increase during the resolution of acute inflammatory response or during the wound healing phase =-=[21, 22]-=-. Neither granulocytes nor dendritic cells express significant levels of CD163. Expression of CD163 also depends on the maturation stage of monocytes/macrophages. To date, only one monocytic cell line...

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...re divided according to their expression of the endotoxin receptor (CD14) and the high affinity immunoglobulin G receptor type III (FcgRIII — CD16), four different subpopulations can be distinguished =-=[18, 19]-=-. The highest expression of CD163 is found on CD14highCD16+ and the lowest on CD14lowCD16– cells [18, 19]. Cells in the CD14highCD16+ subpopulation have been reported to exert predominantly anti-infla...

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...les have been used to identify those subpopulations. Recently, CD163 has been proposed to be a specific marker of monocytes/macrophages cell populations exhibiting strong anti-inflammatory properties =-=[4]-=-. Although CD163 is a marker of anti-inflammatory monocytes/macrophages, it also transduces signals upon binding of its ligands that lead to release of anti-inflammatory mediators such as interleukin-...

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...protein CD163 gene expression is tightly regulated in both a tissue-specific and a differentiation-specific manner [8, 12]. It is detectable as both a cell surface receptor and also as a soluble form =-=[13]-=-. Cellular expression of CD163 is restricted to monocytes and macrophages [8, 12]. Freshly isolated peripheral blood monocytes express a relatively low level of CD163, but this expression increases wi...

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...ted expression of CD163 on 5% or 30% of freshly isolated monocytes, respectively [14, 15]. More recent reports, however, have demonstrated CD163 expression on a majority of peripheral blood monocytes =-=[16, 17]-=-. The discrepancies in reported expression of CD163 on freshly isolated peripheral blood monocytes may be explained by the application of different antibodies and by different techniques used for mono...

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...ophages, with the exception of lymphoid follicle macrophages, express CD163 on their surfaces and the expression is particularly high on liver Kupffer cells and on peritoneal and alveolar macrophages =-=[12, 20]-=-. The level of expression of CD163 on tissue macrophages has been shown to increase during the resolution of acute inflammatory response or during the wound healing phase [21, 22]. Neither granulocyte...

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...nists [28]. Activation of intracellular TLRs does not, however, affect CD163 expression. Other factors which down-regulate CD163 expression include hypoxia and crosslinking of Fcgamma receptor (FcgR) =-=[34, 35]-=-. Hypoxia leads to inhibition of CD163 at the transcriptional level, while cross-linking of FcgR results in shedding of CD163 from the cell surface [34, 35]. Immunoglobulin G immobilized on a culture ...

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... [65]. The associations between T cell proliferation and CD163 also come from in vivo studies in which elevated tissue expression of sCD163 is found in places where T cell proliferation is attenuated =-=[66]-=-. In par372 K Kowal et al. ©Polish Society for Histochemistry and Cytochemistry Folia Histochem Cytobiol. 2011 10.5603/FHC.2011.0052 www.fhc.viamedica.pl ticular, in patients with rheumatoid arthritis...

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...ovial fluids [4]. It contains most of the extracellular part of the membrane CD163, including all SRCR domains [4]. Gene structure The CD163 gene is located on the short arm of chromosome 12 (p13.31) =-=[7]-=-. A gene encoding CD163 molecule-like 1 is also located in the same region close to CD163. The CD163 molecule-like 1 (CD163-L1) gene is highly homologous to the CD163 gene and has the same orientation...

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...ent 1s and 1r, tumor necrosis factor receptor-1, lymphotoxin-beta receptor, alpha2-macroglobulin, CD9, CD27, and CD69 [7]. The CD163 gene spans more than 35 kb and consists of 17 exons and 16 introns =-=[7, 8]-=- (Figure 1). The first ATG codon is located in exon 1, and that exon also contains the N-terminal part of the signal peptide. The remaining parts of the signal peptide are encoded by exon 2 and the fi...

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...d some of them may encode truncated CD163 protein [7, 8]. No functional role for these individual CD163 splice variants has yet been described [7, 8]. Murine CD163 is highly homologous to human CD163 =-=[10]-=-. The gene encoding mouse CD163 is located on chromosome 6 in close proximity to complement components 1r and 1s and to CD9 [11]. That location is homologous to the gene cluster on human chromosome 12...

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...lso seen among swine, rat, monkey and human CD163 receptors [4]. Expression of CD163 protein CD163 gene expression is tightly regulated in both a tissue-specific and a differentiation-specific manner =-=[8, 12]-=-. It is detectable as both a cell surface receptor and also as a soluble form [13]. Cellular expression of CD163 is restricted to monocytes and macrophages [8, 12]. Freshly isolated peripheral blood m...

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...hages, but also dampen IL-10- or glucocorticoid-induced CD163 expression [16]. Surprisingly, transforming growth factor-beta (TGF-b), which is an anti-inflammatory mediator, inhibits CD163 expression =-=[30]-=-. Growth factors which induce differentiation of monocytes into macrophages, such as macrophage colony stimulating factor (M-CSF), enhance CD163 expression, while those inducing differentiation of mon...

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...of tissue macrophages [13, 40–44]. Moreover, detectable levels of sCD163 in body fluids such as the synovial fluid of patients with rheumatoid arthritis or with spondyloarthropathy have been reported =-=[36, 45]-=-. The main mechanism responsible for the appearance of sCD163 in body fluids is thought to be shedding of CD163 from the cell surface of mononuclear phagocytes [29, 32]. At least two enzymes have been...

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...lammatory cytokines. CD163 binds not only to endogenous but also to exogenous ligands such as bacteria and viruses [56–58]. Gram-positive and gram-negative bacteria have each been shown to bind CD163 =-=[56]-=-. CD163 expressed on cell membrane as well as an immobilized protein efficiently binds bacteria. A peptide motif, GRIEIKFQGRW, located within the second SRCR domain of CD163, has been shown to be the ...

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.... A series of mutation and genetic recombination studies have demonstrated that the fifth, but not the first, second or ninth, SRCR domain of CD163 is crucial for binding and internalization of PPRSV =-=[62]-=-. Altogether, studies strongly support the notion that membrane-bound CD163 functions as a receptor for endogenous and exogenous ligands, thereby participating in the initiation and/or perpetuation of...

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...alveolar macrophages [12, 20]. The level of expression of CD163 on tissue macrophages has been shown to increase during the resolution of acute inflammatory response or during the wound healing phase =-=[21, 22]-=-. Neither granulocytes nor dendritic cells express significant levels of CD163. Expression of CD163 also depends on the maturation stage of monocytes/macrophages. To date, only one monocytic cell line...

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...ocyte/macrophage CD163 expression after shedding of the receptor in response to Toll like receptor (TLR) stimulation [27, 28]. Glucocorticoids are at least equally potent inducers of CD163 expression =-=[16, 26]-=-. The magnitude of up-regulation of CD163 expression depends on the potency of the glucocorticoid: those having the greatest affinity for the glucocorticoid receptor are the most potent for up-regulat...

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...y monocytes/macrophage cells [28]. This down-regulation of CD163 expression is caused by shedding of CD163 from the cell surface, which has been shown to involve a metalloproteinase-dependent process =-=[29, 32]-=-. The same mechanism is responsible for down-regulation of monocyte CD163 expression by oxidative stress or 8-iso-prostaglandin F2a [33]. Prolonged stimulation with cell membrane TLR agonists, however...

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...e form, as membrane-bound CD163 does not exert such an effect [64]. The interaction between sCD163 and T lymphocytes is mediated by binding of sCD163 to non-muscle myosin heavy chain in T lymphocytes =-=[65]-=-. The associations between T cell proliferation and CD163 also come from in vivo studies in which elevated tissue expression of sCD163 is found in places where T cell proliferation is attenuated [66]....

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...lar metabolism within the lysosomes [52]. The heme undergoes intracellular degradation by the rate-limiting enzyme heme oxygenase-1 (HO-1), giving rise to free iron, biliverdine and carbon oxide (CO) =-=[49, 53]-=-. Altogether, the interaction of Hb-Hp with CD163 leads to release of IL-10 and CO, which exert strong anti-inflammatory effects. The release of IL-10 and CO by macrophages in response to binding of H...

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... a combinatorial peptide library designed to search for a tumor necrosis factor-like weak inducer of apoptosis (TWEAK, TNFS12) ligands led to the discovery of motifs similar to those present in CD163 =-=[54]-=-. The discovery was reinforced by direct protein-protein interaction experiments, which showed that TWEAK specifically binds to CD163 [54]. TWEAK is a member of the TNF superfamily and plays many impo...

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...roliferation, apoptosis and angiogenesis [59]. Its ability to regulate innate and adaptive immune response seems to be one of the most interesting aspects of TWEAK from an immunological point of view =-=[60]-=-. In mice with genetically silenced TWEAK (TWEAK –/–), systemic administration of LPS results in a stronger inflammatory response with greater production of IFN-g and IL-12, but with less IL-10 than i...

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...nists [28]. Activation of intracellular TLRs does not, however, affect CD163 expression. Other factors which down-regulate CD163 expression include hypoxia and crosslinking of Fcgamma receptor (FcgR) =-=[34, 35]-=-. Hypoxia leads to inhibition of CD163 at the transcriptional level, while cross-linking of FcgR results in shedding of CD163 from the cell surface [34, 35]. Immunoglobulin G immobilized on a culture ...

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...3 on skin macrophages and peripheral blood monocytes from patients with systemic sclerosis (scleroderma), an autoimmune disease characterized by local inflammatory infiltrates and widespread fibrosis =-=[68]-=-. The role of increased CD 163 in the pathogenesis of systemic sclerosis remains to be established. Perspectives Evaluation of CD163 expression would appear to be an interesting avenue in the assessme...

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...of tissue macrophages [13, 40–44]. Moreover, detectable levels of sCD163 in body fluids such as the synovial fluid of patients with rheumatoid arthritis or with spondyloarthropathy have been reported =-=[36, 45]-=-. The main mechanism responsible for the appearance of sCD163 in body fluids is thought to be shedding of CD163 from the cell surface of mononuclear phagocytes [29, 32]. At least two enzymes have been...

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...ry, asthmatic patients who did not develop late asthmatic response after allergen challenge were characterized by elevated concentrations of plasma sCD163 and an increase in monocyte CD163 expression =-=[37]-=-. Resolution of inflammatory response after allergen exposure is, therefore, associated with high plasma sCD163 concentrations, which is in line with original descriptions of elevated CD163 expression...

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... be the main mechanism affecting sCD163 levels. Intravenous administration of hydrocortisone to healthy volunteers resulted in enhanced CD163 mRNA and protein expression on peripheral blood monocytes =-=[46, 47]-=-. Elevated numbers of CD163+ monocytes have been seen as soon as six hours after intravenous administration of glucocorticoids, and lasted for at least four days [46]. The maximum effect was seen betw...

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... be the main mechanism affecting sCD163 levels. Intravenous administration of hydrocortisone to healthy volunteers resulted in enhanced CD163 mRNA and protein expression on peripheral blood monocytes =-=[46, 47]-=-. Elevated numbers of CD163+ monocytes have been seen as soon as six hours after intravenous administration of glucocorticoids, and lasted for at least four days [46]. The maximum effect was seen betw...

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...istochemica et Cytobiologica 2011, Vol. 49, No. 3, 365–374) Key words: CD163, inflammation Introduction Monocytes and macrophages play an important role in the regulation of the inflammatory response =-=[1, 2]-=-. Based on their functional properties, at least two subpopulations (M1 and M2) of mononuclear phagocytes, which differ in their pro- and anti-inflammatory potential, have been described [3]. The cell...

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...ation with protein kinase C and creatine kinase [4]. CD163 is heavily glycosylated with N-linked glycans. Treatment of CD163 with endoglycosidase F significantly reduces the molecular weight of CD163 =-=[6]-=-. Moreover, CD163 also exists as a soluble protein (sCD163) [4]. It is detectable in the plasma of healthy persons and can also be detected in body fluids such as synovial fluids [4]. It contains most...

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...been described [7, 8]. Murine CD163 is highly homologous to human CD163 [10]. The gene encoding mouse CD163 is located on chromosome 6 in close proximity to complement components 1r and 1s and to CD9 =-=[11]-=-. That location is homologous to the gene cluster on human chromosome 12p13.3, which contains the human CD163 gene. Like human CD163, mouse CD163 is a type I transmembrane protein which contains a sho...

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... IL-1a, IL-1b or chemokines such as CXCL-8 (IL-8) decrease expression of CD163 [16]. Similarly, exogenous pro-inflammatory molecules such as lipopolysaccharide (LPS) also decrease expression of CD163 =-=[28, 29]-=-. Interestingly, not only a Th-1 type cytokine (interferon-gamma; IFN-g) but also Th-2 type cytokines (IL-4 and IL-13) down-regulate CD163 expression [16]. These cytokines can suppress not only up-reg...

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...exerts pro- and anti-inflammatory effects on mononuclear phagocytes, enhances expression of CD163 [18]. Several chemokines have also been reported to affect CD163 expression on mononuclear phagocytes =-=[16, 31]-=-. CCL-3 (MIP-1a) and CXCL-8 down-regulate spontaneous and glucocorticoid-induced CD163 expression on cultured human monocytes [16]. Monocytes cultured in vitro in the presence of CXCL-4 express less C...

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...n association between plasma MMP-9 levels and plasma sCD163 concentrations has been demonstrated in multiple sclerosis patients, supporting a role of MMP-9 in the regulation of CD163 shedding in vivo =-=[38]-=-. Several alternative splice variants of CD163 mRNA, which code for truncated forms of CD163 protein, have been reported. The transcriptional and/or translational regulation of CD163 expression does n...

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...hen released from erythrocytes, Hb binds to Hp to form complexes containing at least two Hb molecules. Formation of these complexes results in exposure of a new epitope, which allows binding to CD163 =-=[50, 51]-=-. The binding site for Hb-Hp complexes is located within the 3 SRCR domain, and the binding process is both a calciumand pH-dependent phenomenon [50, 51]. When calcium concentration is below 0.5 mM, o...

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...163 complex is internalized and Hb-Hp is delivered to early endosomes, where CD163 dissociates and recycles to the plasma membrane, while Hb-Hp undergoes intracellular metabolism within the lysosomes =-=[52]-=-. The heme undergoes intracellular degradation by the rate-limiting enzyme heme oxygenase-1 (HO-1), giving rise to free iron, biliverdine and carbon oxide (CO) [49, 53]. Altogether, the interaction of...

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...including fibroblasts, endothelial cells and epithelial cells, release a broad range of chemokines, pro-inflammatory cytokines and matrix metalloproteinases (MMPs) in response to stimulation by TWEAK =-=[57]-=-. Monocytes express little or no Fn14 [54, 59]. They do, however, bind specifically TWEAK, and CD163 is responsible for that binding [54]. Further experiments revealed that the TWEAK binding site on C...

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...eptibility to infection for both viruses is proportional to the expression of CD163 on the cell surface [57, 58], and the viruses have a very restricted cell tropism for the monocyte/macrophage cells =-=[57, 58, 61]-=-. In a study of swine bone marrow monocyte precursors, peripheral blood monocytes and alveolar macrophages, the susceptibility of infection by ASFV was dependent on the degree of maturation of mononuc...

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...o allergen challenge. In chronic obstructive pulmonary disease (COPD), substantial expression of CD163 has been demonstrated on macrophages derived from bronchoalveolar lavage (BAL) or induced sputum =-=[67]-=-. Smoking cessation leads polarization of macrophages towards an anti-inflammatory phenotype, which is reflected by a higher percentage of macrophages expressing CD163 in BAL derived from ex-smokers. ...