Dendritic cells (DCs) get their name from their surface projections (that resemble the dendrites of neurons — see figure).
They are found in most tissues of the body and are particularly abundant in those that are interfaces between the external and internal environments, e.g., skin and the lining of the gastrointestinal tract, where they are ideally placed to encounter invading pathogens.
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| Two dendritic cells (arrows) from the spleen of a mouse. Compare their smooth surface with that of the two macrophages visible at the upper left. (Courtesy of Ralph Steinman, from R. M. Steinman et al., J. Exp. Med. 149:1, 1979.) |
In either case, the ingested antigens are degraded in lysosomes into peptide fragments that are then displayed at the cell-surface nestled in MHC molecules [Link].
| (Dendritic cells can also present undegraded antigen to B cells; that is, antigen that has not been processed into peptide/MHC complexes — Link.) |
Having ingested antigen in the tissue, they migrate to lymph nodes and spleen where they can meet up with T cells bearing the appropriate T-cell receptor for antigen (TCR).
What happens next depends on the nature of the antigen.What accounts for the activation of dendritic cells by foreign antigens but not by self antigens?
Pathogens, especially bacteria, have molecular structures thatExamples:
Dendritic cells have a set of transmembrane receptors that recognize different types of PAMPs. These are called Toll-like receptors (TLRs) because of their homology to receptors first discovered and named in Drosophila.
TLRs identify the nature of the pathogen and turn on an effector response appropriate for dealing with it. These signaling cascades lead to the expression of various cytokine genes.
Under other circumstances, activated dendritic cells may secrete IL-10, leading to the formation of regulatory T cells (Treg and Tr1) that dampen immune responses.
While all DCs share certain features, they actually represent a variety of cell types with different differention histories, phenotypic traits and, as outlined above, different effector functions.
Examples:
These cells get their name from their extensive endoplasmic reticulum which resembles that of plasma cells. However, unlike plasma cells that are machines for pumping out antibodies, these dendritic cells produce huge amounts of interferons (alpha and beta). They do so in response to viral infections.
Plasmacytoid DCs have toll-like receptors on their surface:DC1 DCs present antigen to helper T cells of the Th1 subset. This subset secretes large amounts of IL-12 [View]. It is this subset that mediates cell-mediated immune responses like the allergic response to poison ivy.
DC2 DCs present antigen to helper T cells of the Th2 subset — the subset responsible for providing help to B cells, including those that secrete antibodies that trigger IgE-mediated allergic responses (e.g. to ragweed pollen).
![]() | Phase contrast micrograph of spleen cells after 2 days in culture. Four dendritic cells (arrows) can be seen clustered with lymphocytes. (Courtesy of Ralph Steinman from K. Inaba et al., J. Exp. Med. 160:858, 1984.) |
Ralph Steinman, the pioneer in the study of dendritic cells, has provided striking visual evidence of the cellular interactions between antigen-presenting dendritic cells, T cells, and B cells. When spleen cells are cultured with antigen, tight clusters of cells form (see figure). The clustering occurs in two phases:
Some dendritic cells not only activate T cells to respond to a particular antigen but tell them where to go to deal with that antigen.
Two examples:
(In telling this story, I cannot help being reminded of the way that scout bees, having found food, return to the hive and tell the worker bees there where to go to find it! [Link])
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