Autocrine Type I IFN and Contact with Endothelium Promote the Presentation of Influenza A Virus by Monocyte-Derived APC

Qu, Chunfeng; Moran, Thomas M.; Randolph, Gwendalyn J.

doi:10.4049/jimmunol.170.2.1010

Cited by 20 publications

(31 citation statements)

References 40 publications

(47 reference statements)

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“…Thus, the inflammatory milieu induced by M. tuberculosis might be enriched with IFN-␣ that, in turn, could favor the differentiation of recruited monocytes into DCs (40). The autocrine secretion of IFN-␣ has also been suggested to be a modulator of monocyte differentiation in a model tissue setting in which monocytes were cocultured with endothelium grown on a type I collagen matrix (35). In this regard, in vivo experiments clearly indicated that M. tuberculosis strains with the ability to induce IFN-␣ displayed increased virulence and a capacity to induce disease (26,27).…”

Section: Discussionmentioning

confidence: 99%

Mycobacterium tuberculosisDiverts Alpha Interferon-Induced Monocyte Differentiation from Dendritic Cells into Immunoprivileged Macrophage-Like Host Cells

et al. 2004

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Section: Discussionmentioning

confidence: 99%

Mycobacterium tuberculosisDiverts Alpha Interferon-Induced Monocyte Differentiation from Dendritic Cells into Immunoprivileged Macrophage-Like Host Cells

et al. 2004

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“…However, we have found that this is stimulus dependent and that, when appropriately stimulated, nonplasmacytoid mouse DC also produce high amounts of IFN␣. 5 Similarly, nonplasmacytoid human monocyte-derived DC produce type I IFN in response to infection with influenza (43,44).…”

Section: Endritic Cells (Dc)mentioning

confidence: 99%

Relationships Among Murine CD11chigh Dendritic Cell Subsets as Revealed by Baseline Gene Expression Patterns

Edwards

Chaussabel

Tomlinson

et al. 2003

The Journal of Immunology

120

119

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The functional relationships and properties of different subtypes of dendritic cells (DC) remain largely undefined. To better characterize these cells, we used global gene analysis to determine gene expression patterns among murine CD11chigh DC subsets. CD4+, CD8α+, and CD8α− CD4− (double negative (DN)) DC were purified from spleens of normal C57/BL6 mice and analyzed using Affymetrix microarrays. The CD4+ and CD8α+ DC subsets showed distinct basal expression profiles differing by >200 individual genes. These included known DC subset markers as well as previously unrecognized, differentially expressed CD Ags such as CD1d, CD5, CD22, and CD72. Flow cytometric analysis confirmed differential expression in nine of nine cases, thereby validating the microarray analysis. Interestingly, the microarray expression profiles for DN cells strongly resembled those of CD4+ DC, differing from them by <25 genes. This suggests that CD4+ and DN DC are closely related phylogenetically, whereas CD8α+ DC represent a more distant lineage, supporting the historical distinction between CD8α+ and CD8α− DC. However, staining patterns revealed that in contrast to CD4+ DC, the DN subset is heterogeneous and comprises at least two subpopulations. Gene Ontology and literature mining analyses of genes expressed differentially among DC subsets indicated strong associations with immune response parameters as well as cell differentiation and signaling. Such associations offer clues to possible unique functions of the CD11chigh DC subsets that to date have been difficult to define as rigid distinctions.

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“…In patients with lupus, there is an association between disease activity and type I IFN levels in the peripheral blood [24][25][26][27]. Not all lupus patients have measurably increased levels of type 1 IFN, but they may have increased type 1 IFN-responsive gene expression "signatures" in blood mononuclear cells [16,18]. This suggests that these cells have been exposed to high levels of type 1 IFN elsewhere (e.g., in the tissues).…”

Section: Clinical Discussionmentioning

confidence: 99%

“…In both disorders the lymph node pathology can show histiocytic necrotizing lymphadenitis, and in both, the plasmacytoid histiocyte or PDC plays a role. In the lymph node, PDCs are localized to the "T zone," which is centered around the high endothelial venules [15], where they also present antigen [16]. The pathology in KFD often centers around T zone of the lymph node [17], although in this case, the lymph node architecture was not preserved and the T zone was not clearly seen.…”

Section: Clinical Discussionmentioning

confidence: 99%

Overlap between Systemic Lupus Erythematosus and Kikuchi Fujimoto Disease

Gordon

Magro

et al. 2009

HSS Journal®

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Autocrine Type I IFN and Contact with Endothelium Promote the Presentation of Influenza A Virus by Monocyte-Derived APC

Cited by 20 publications

References 40 publications

Mycobacterium tuberculosisDiverts Alpha Interferon-Induced Monocyte Differentiation from Dendritic Cells into Immunoprivileged Macrophage-Like Host Cells

Mycobacterium tuberculosisDiverts Alpha Interferon-Induced Monocyte Differentiation from Dendritic Cells into Immunoprivileged Macrophage-Like Host Cells

Relationships Among Murine CD11chigh Dendritic Cell Subsets as Revealed by Baseline Gene Expression Patterns

Overlap between Systemic Lupus Erythematosus and Kikuchi Fujimoto Disease

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