Characterization of sheep afferent lymph dendritic cells and their role in antigen carriage.

Bujdoso, Raymond; Hopkins, John; Dutia, Bernadette M.; Young, Patricia A.; McConnell, Ian

doi:10.1084/jem.170.4.1285

Cited by 184 publications

(89 citation statements)

References 40 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Fossum (32) reported that purified lymph DC injected into footpads of mice mostly were retained at the site of injection. Lymph DC represent a maturing DC population (33), and hence these findings may be consistent with our results. More recently, Ag-stimulated blood-derived human DC used therapeutically in human cancer patients were only partially cleared from an i.d.…”

Section: Cd86supporting

confidence: 82%

Maturation and Trafficking of Monocyte-Derived Dendritic Cells in Monkeys: Implications for Dendritic Cell-Based Vaccines

et al. 2000

The Journal of Immunology

137

View full text Add to dashboard Cite

Human dendritic cells (DC) have polarized responses to chemokines as a function of maturation state, but the effect of maturation on DC trafficking in vivo is not known. We have addressed this question in a highly relevant rhesus macaque model. We demonstrate that immature and CD40 ligand-matured monocyte-derived DC have characteristic phenotypic and functional differences in vitro. In particular, immature DC express CC chemokine receptor 5 (CCR5) and migrate in response to macrophage inflammatory protein-1α (MIP-1α), whereas mature DC switch expression to CCR7 and respond exclusively to MIP-3β and 6Ckine. Mature DC transduced to express a marker gene localized to lymph nodes after intradermal injection, constituting 1.5% of lymph node DC. In contrast, cutaneous DC transfected in situ via gene gun were detected in the draining lymph node at a 20-fold lower frequency. Unexpectedly, the state of maturation at the time of injection had no influence on the proportion of DC that localized to draining lymph nodes, as labeled immature and mature DC were detected in equal numbers. Immature DC that trafficked to lymph nodes underwent a significant up-regulation of CD86 expression indicative of spontaneous maturation. Moreover, immature DC exited completely from the dermis within 36 h of injection, whereas mature DC persisted in large numbers associated with a marked inflammatory infiltrate. We conclude that in vitro maturation is not a requirement for effective migration of DC in vivo and suggest that administration of Ag-loaded immature DC that undergo natural maturation following injection may be preferred for DC-based immunotherapy.

show abstract

Section: Cd86supporting

confidence: 82%

Maturation and Trafficking of Monocyte-Derived Dendritic Cells in Monkeys: Implications for Dendritic Cell-Based Vaccines

et al. 2000

The Journal of Immunology

137

View full text Add to dashboard Cite

show abstract

“…10 Although DC efflux from tissues to the tissue-draining LN is difficult to accurately quantify, 11 it is clear that tissue-DC homeostasis requires constant replacement with new cells. BM chimera studies in mice established that kidney and heart DCs are replaced in 2 to 4 weeks after lethal irradiation and BM transplantation, whereas DC repopulation in the vagina, 12 airway epithelia, 13 and the gut is more rapid and occurs in 7 to 13 days (M. Bogunovic and M.M., unpublished data, January 2009).…”

Section: Dcs In Nonlymphoid Tissuesmentioning

confidence: 99%

Dendritic cell homeostasis

Mérad

Manz

2009

Blood

333

356

View full text Add to dashboard Cite

IntroductionDendritic cells (DCs) are hematopoietic cells that belong to the antigen-presenting cell (APC) family, which also includes B cells and macrophages. Although Langerhans cells (LCs) in the skin were described in 1868, the role of DCs as APCs was not appreciated until 1973, when Steinman and Cohn first identified DCs in mouse spleen as potent stimulators of the primary immune response. 1 Shortly thereafter, several groups reported the presence of DCs in nonlymphoid tissues of rodents and humans and demonstrated early evidence that these cells contribute to heart and kidney transplantation rejection. 2 However, the low number of DCs in vivo, the paucity of markers that distinguish them from monocytes/macrophages, and the problems in purifying these cells made for slow progress. In the 1990s, the development of methods to isolate and generate DCs from blood and bone marrow (BM) led to explosive growth of the DC field. [3][4][5] Studies in the last decade have established the critical role of DCs in the maintenance of immunologic integrity and their importance in the development and potential treatment of human disease, leading in 2007 to the attribution of the Albert Lasker Award for Basic Medical Research to Dr Ralph Steinman (Rockefeller University, New York, NY) in recognition of his discovery of DCs. Heterogeneity, localization, and life cycle of DC populationsDCs are a heterogeneous population of cells that can be divided into 2 major populations: (1) nonlymphoid tissue migratory and lymphoid tissue-resident DCs and (2) plasmacytoid DCs (pDCs, also called natural interferon-producing cells). The term "classic" or "conventional" DCs (cDCs) has recently been used to oppose lymphoid organ-resident DCs to pDCs. Nonlymphoid organ DCs, on the other hand, are mainly called tissue DCs. Although the term cDC is helpful in some respect, it also might be confusing as nonlymphoid tissue DCs are also different from pDCs, and primary nonlymphoid tissue DCs can be found in lymph nodes (LNs) on migration but are not cDCs. Thus, throughout this review, the term DCs will refer to all non-pDCs whether they are present in lymphoid or nonlymphoid tissues, and location will be appropriately specified.Migratory and resident DCs have 2 main functions: the maintenance of self-tolerance and the induction of specific immune responses against invading pathogens, 1,6 whereas the main function of pDCs is to secrete paramount amounts of interferon-␣ in response to viral infections and to prime T cells against viral antigens. 7 Figure 1 and Table S1 (available on the Blood website; see the Supplemental Materials link at the top of the online article) show different DC populations, their frequencies, locations, and turnover in various lympoid and nonlymphoid tissues. DCs in nonlymphoid tissuesNonlymphoid tissue DCs can be distinguished between those present in sterile tissues, such as the pancreas and the heart, DCs present in filtering sites, such as the liver and the kidney, and DCs present at environmental interfaces as lung, gut...

show abstract

“…Following exposure to antigen, dendritic cells mature and develop potent immunostimulatory activity whilst migrating to draining lymph nodes; there they interact with T cells to initiate T cell responses. Thus, in various animal models, dendritic cells in the afferent lymph are associated with antigen and can initiate antigen-specific T cell-mediated responses [3,26,27].…”

Section: Figmentioning

confidence: 99%

Distribution of human colonic dendritic cells and macrophages

Pavli

Maxwell

Pol

et al. 1996

Clinical and Experimental Immunology

View full text Add to dashboard Cite

SUMMARYTo define the phenotype of intestinal dendritic cells and macrophages, resected colonic specimens were used to obtain lamina propria cell suspensions by EDTA treatment, then enzymatic digestion. The phenotype of dendritic cell-enriched suspensions was compared with that of macrophage-enriched populations by immunocytochemistry using the avidin-biotin-peroxidase (ABC) system and immunoelectron microscopy. Dendritic cells expressed HLA-DR (L243) and HLA-DQ-associated (RFD1) antigens and CD68 in a perinuclear distribution. Staining for S100 was weak or absent. Macrophages also expressed HLA markers (L243 and RFD1) and CD68. The 25F9 antigen was expressed strongly, whilst CD14 was absent from cells isolated from non-inflamed tissues. To determine their anatomic distribution, immunohistochemistry was performed using single-and double-labelling techniques (ABC

show abstract

Characterization of sheep afferent lymph dendritic cells and their role in antigen carriage.

Cited by 184 publications

References 40 publications

Maturation and Trafficking of Monocyte-Derived Dendritic Cells in Monkeys: Implications for Dendritic Cell-Based Vaccines

Maturation and Trafficking of Monocyte-Derived Dendritic Cells in Monkeys: Implications for Dendritic Cell-Based Vaccines

Dendritic cell homeostasis

Distribution of human colonic dendritic cells and macrophages

Contact Info

Product

Resources

About