Heparin Induces Differentiation of CD1a+ Dendritic Cells from Monocytes: Phenotypic and Functional Characterization

Xia, Chang-Qing; Kao, Kuo-Jang

doi:10.4049/jimmunol.168.3.1131

Cited by 36 publications

(47 citation statements)

References 43 publications

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“…This finding underscores the basis for the ineffectiveness of anti-IL-10 Ab to enhance Th1 induction via binding and neutralization of secreted IL-10. A recent study suggested the reverse relationship between the production of IL-10 and IL-12 in activated DC [30], a finding also observed in the current study. Neutralization of the secreted IL-10 by Ab and IL-10 antisense oligodNTP could enhance the production of IL-12 [31].…”

Section: Discussionsupporting

confidence: 89%

Small interference RNA modulation of IL‐10 in human monocyte‐derived dendritic cells enhances the Th1 response

Liu

Akasaki

et al. 2004

Eur J Immunol

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RNA interference technology has been used to modulate dendritic cell (DC) function by targeting the expression of genes such as IL-12 and NF-kB. In this paper, we demonstrate that transfection of DC with IL-10-specific double strands of small interference RNA (siRNA) resulted in potent suppression of IL-10 gene expression without inducing DC apoptosis or blocking DC maturation. Inhibition of IL-10 by siRNA was accompanied by increased CD40 expression and IL-12 production after maturation, which endowed DC with the ability to significantly enhance allogeneic T cell proliferation. IL-10 siRNA transfection did not affect MHC class II, CD86, CD83, or CD54 expression in mature DC. To further test the ability of IL-10 siRNA-treated DC to induce a T cell response, naive CD4 T cells were stimulated by autologous DC pulsed with KLH. The results indicated that IL-10 siRNA-transfected DC enhanced Th1 responses by increasing IFN-+ and decreasing IL-4 production. These findings suggest the potential for a novel immunotherapeutic strategy of using IL-10 siRNAtransfected antigen-presenting cells as vaccine delivery agents to boost the Th1 response against pathogens and tumors that are controlled by Th1 immunity.

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Section: Discussionsupporting

confidence: 89%

Small interference RNA modulation of IL‐10 in human monocyte‐derived dendritic cells enhances the Th1 response

Liu

Akasaki

et al. 2004

Eur J Immunol

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“…Cellular Effects. GAGs display complex biological activities toward various cells, including lymphocytes, monocytes, dendritic, and stromal cells (10,17,(20)(21)(22)(23). We examined cellular responses to GAGs to identify a correlation with disease development in mice.…”

Section: Resultsmentioning

confidence: 99%

Glycosaminoglycans are a potential cause of rheumatoid arthritis

Wang

Roehrl²

2002

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

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Rheumatoid arthritis (RA) is a chronic, systemic, and inflammatory disease of connective tissue with unknown etiology. We investigated whether aberrant immune responses to glycosaminoglycans (GAGs), a major component of joint cartilage, joint fluid, and other soft connective tissue, causes this disease. Here we show that injection of GAGs such as hyaluronic acid, heparin, and chondroitin sulfates A, B, and C induce arthritis, tendosynovitis, dermatitis, and other pathological conditions in mice. We developed a technique by staining tissue specimens with fluorochrome-or biotin-labeled GAGs to visualize the direct binding between cells and GAGs. We discovered that inflammatory infiltrates from the affected tissue are dominated by a distinct phenotype of GAG-binding cells, a significant portion of which are CD4 ؉ T cells. GAG-binding cells seem to be expanded in bone marrow of GAG-immunized mice. Furthermore, we identified GAG-binding cells in inflamed synovial tissue of human patients with RA. Our findings suggest that carbohydrate self-antigenic GAGs provoke autoimmune dysfunctions that involve the expansion of GAG-binding cells which migrate to anatomical sites rich in GAGs. These GAG-binding cells might, in turn, promote the inflammation and pathology seen both in our murine model and in human RA.

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“…40,41 Our monocyte-derived DCs generated in culture with GM-CSF and IL-4 in the presence of FCS were CD1a ϩ and showed a typical phenotype of intermediate maturity expressing low levels of CD83. 42,43 In addition, these DCs showed a strong tendency for further maturation as shown by the rapid increase in CD83 ϩ DCs after a 4-hour pulsing with KLH. Lipopolysaccharides (LPS), which are notably present in FCS, may contribute, through the engagement of pattern recognition receptor TLR-4, to drive resting monocyte-derived DCs into the DC1 development pathway.…”

Section: Discussionmentioning

confidence: 99%

Intranodal injection of semimature monocyte-derived dendritic cells induces T helper type 1 responses to protein neoantigen

Gilliet

Kleinhans

Lantelme

et al. 2003

Blood

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Heparin Induces Differentiation of CD1a+ Dendritic Cells from Monocytes: Phenotypic and Functional Characterization

Cited by 36 publications

References 43 publications

Small interference RNA modulation of IL‐10 in human monocyte‐derived dendritic cells enhances the Th1 response

Small interference RNA modulation of IL‐10 in human monocyte‐derived dendritic cells enhances the Th1 response

Glycosaminoglycans are a potential cause of rheumatoid arthritis

Intranodal injection of semimature monocyte-derived dendritic cells induces T helper type 1 responses to protein neoantigen

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