Mast cell modulation of neutrophil influx and bacterial clearance at sites of infection through TNF-α

Malaviya, Ravi; Ikeda, Teruo; Ross, Elaine; Abraham, Soman N.

doi:10.1038/381077a0

Cited by 1,021 publications

(896 citation statements)

References 22 publications

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“…The ability of gp49B1 to suppress the mast cell response to activating concentrations of soluble SCF is consistent with the biologic necessity for mast cells to respond fully to the basal concentrations of SCF that mediate their development and survival in vivo [21] so as to provide intact cells that protect against bacterial infections [22][23][24][25][26]. The hyperresponsive phenotype in gp49B -/-mice was not the result of an abnormal level of endogenous SCF, because naïve gp49B -/-mice had normal numbers of mast cells not only in the ear [4], but also in the tongue, heart, lung, and small intestine (data not shown), indicating that the SCF-dependent, systemic development of mast cells is not negatively regulated by gp49B1.…”

Section: Effects Of Receptor Antagonists For Mast Cell Granule-derivesupporting

confidence: 53%

“…The cytokine stem cell factor (SCF) is mandatory for normal mast cell development; mice of the WBB6F1-Kit W /Kit W-v strain that have a dysfunctional form of the SCF receptor (c-kit) have essentially no tissue mast cells [21]. These mice are more susceptible to death when subjected to a microbial challenge such as acute septic peritonitis, but they can be protected by adoptive transfer of normal mast cells, an effect that is enhanced when mast cell development in vivo is amplified by provision of exogenous SCF [22][23][24][25][26]. Thus, SCF produced by both stromal and hematopoietic cells [27] provides a host resistance function that is mediated through maintenance of mast cell numbers in peripheral tissues.…”

Section: Introductionmentioning

confidence: 99%

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gp49B1 suppresses stem cell factor‐induced mast cell activation‐secretion and attendant inflammation in vivo

et al. 2003

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We report that gp49B1, a mast cell membrane receptor with two immunoreceptor tyrosinebased inhibitory motifs (ITIM), constitutively inhibits mast cell activation-secretion induced by stem cell factor (SCF), a tissue-derived cytokine that also regulates mast cell development. The intradermal injection of SCF into the ears of gp49B1 null (gp49B -/-) mice elicited 4-and 2.5-fold more degranulating mast cells and tissue swelling caused by edema, respectively, than in gp49B +/+ mice. SCF did not induce tissue swelling in mast cell-deficient mice, and the responsiveness of gp49B -/-mice to mast cell-associated amine and lipid mediators was unaltered. When gp49B +/+ and gp49B -/-mice were pretreated with antagonists of the amines, SCF-induced tissue swelling was reduced by G 90% and 60%, respectively, and it was reduced by G 90% in both genotypes when a cysteinyl leukotriene receptor antagonist was also provided. Hence, the dominant contribution of secretory granule amines to SCF-induced tissue swelling is the result of gp49B1-mediated inhibition of the production of cysteinyl leukotrienes by mast cells. Our findings also provide the first example of an ITIMbearing receptor that constitutively suppresses inflammation generated in vivo independently of the adaptive immune response by a receptor that signals through intrinsic tyrosine kinase activity rather than immunoreceptor tyrosine-based activation motifs.

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Section: Effects Of Receptor Antagonists For Mast Cell Granule-derivesupporting

confidence: 53%

Section: Introductionmentioning

confidence: 99%

gp49B1 suppresses stem cell factor‐induced mast cell activation‐secretion and attendant inflammation in vivo

et al. 2003

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“…Although the dermal cells responsible for recruiting neutrophils following UVB exposure are not known, studies using mast cell deficient mice show that mast cells are critical cellular intermediaries required for the recruitment of neutrophils to sites of inflammation. 84 While direct exposure of cord blood derived mast cells to UVB in vitro causes CXCL8 production in these cells, 85 this is unlikely to be the primary mechanism by which dermal mast cells produce CXCL8 after UV exposure in vivo; rather, we hypothesize that UVB-induced PAF stimulates IL-33 production in fibroblasts that then acts either in an autocrine manner 86 or on neighboring dermal mast cells 23 to induce expression of neutrophil chemoattractants such as CXCL8. In this way, UV-induced IL-33 acts as a novel endogenous danger signal mediating the recruitment of innate immune cells to sites of infection or cellular damage.…”

Section: Discussionmentioning

confidence: 88%

The Immune-Modulating Cytokine and Endogenous Alarmin Interleukin-33 Is Upregulated in Skin Exposed to Inflammatory UVB Radiation

Byrne

Beaugie

O’Sullivan

et al. 2011

The American Journal of Pathology

101

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The cellular and molecular mechanisms by which UV radiation modulates inflammation and immunity while simultaneously maintaining skin homeostasis is complex and not completely understood. Similar to the effects of UV, IL-33 has potent immune-modulating properties that are mediated by the downstream induction of cytokines and chemokines. We have discovered that exposure of mice in vivo or human skin samples ex vivo to inflammatory doses of UVB induced IL-33 expression within the epidermal and dermal skin layers. Using a combination of murine cell lines and primary human cells, we demonstrate that both UV and the oxidized lipid platelet activating factor induce IL-33 expression in keratinocytes and dermal fibroblasts. Highlighting the significance of these results, we found that administering IL-33 to mice in vivo suppressed the induction of Th1-mediated contact hypersensitivity responses. This may have consequences for skin cancer growth because UV-induced squamous cell carcinomas that evade immunological destruction were found to express significantly higher levels of IL-33. Finally, we demonstrate that dermal mast cells and skininfiltrating neutrophils closely associate with UV-induced IL-33-expressing fibroblasts. Our results therefore identify and support a role for IL-33 as an important early danger signal produced in response to inflammation-inducing UV radiation.

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“…MCs release newly generated mediators such as PGD 2 , leukotriene (LT) B 4 or LTC 4 upon activation as well as preformed mediators [3]. We found the tags for enzymes relating to synthesis and degradation of PGD 2 appeared frequently (Table 2), while those involved in synthesizing lipoxygenase products such as LTB 4 or LTC 4 were detected rarely (5-lipoxygenase, zero; LTC 4 synthase, one; and LTA 4 hydrolase, one). This suggests a possibility that PGD 2 is constitutively synthesized and may have some functions in unstimulated MCs.…”

Section: Identi¢cation Of Novel Mc-speci¢c Genesmentioning

confidence: 99%

“…Recent ¢ndings suggest that MCs are also involved in non-allergic processes such as innate immunity by producing high levels of cytokines [4]. However little is known about other roles of MCs.…”

Section: Introductionmentioning

confidence: 99%

Identification of novel mast cell genes by serial analysis of gene expression in cord blood‐derived mast cells

Kuramasu

Kubota

Matsumoto³

et al. 2001

FEBS Letters

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The gene expression profile of human cord bloodderived mast cells (MCs) was investigated using serial analysis of gene expression (SAGE). A total of 22 914 tags, representing 9181 unique transcripts, were sequenced. By selecting tags that were detected more frequently in MCs than in other tissues, genes characteristic of MCs were enriched. Reverse transcription-PCR and the high-density oligonucleotide array hybridization confirmed the validity of our SAGE result. About 70% of the selected genes were previously uncharacterized. Northern blot analysis showed the MC-specific expression of selected genes. This inventory will be useful to identify novel genes with important functions in MCs. ß

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Mast cell modulation of neutrophil influx and bacterial clearance at sites of infection through TNF-α

Cited by 1,021 publications

References 22 publications

gp49B1 suppresses stem cell factor‐induced mast cell activation‐secretion and attendant inflammation in vivo

gp49B1 suppresses stem cell factor‐induced mast cell activation‐secretion and attendant inflammation in vivo

The Immune-Modulating Cytokine and Endogenous Alarmin Interleukin-33 Is Upregulated in Skin Exposed to Inflammatory UVB Radiation

Identification of novel mast cell genes by serial analysis of gene expression in cord blood‐derived mast cells

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