Cross-dressed CD8α
 +
 /CD103
 +
 dendritic cells prime CD8
 +
 T cells following vaccination

Li, Lijin; Kim, Sojung; Herndon, John M.; Goedegebuure, Peter S.; Belt, Brian A.; Satpathy, Ansuman T.; Fleming, Timothy P.; Hansen, Ted H.; Murphy, Kenneth M.; Gillanders, William E.

doi:10.1073/pnas.1203468109

Cited by 63 publications

(47 citation statements)

References 21 publications

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“…This is in striking contrast to antigens delivered by recombinant viruses or bacteria, which can elicit huge responses . An adjuvant that promotes an efficient CD8 + T‐cell response will almost certainly need to act via cross‐presenting or cross‐dressing DCs and, in this respect, CD103 + dDCs are prime candidates . It is therefore important to understand the effects of adjuvants on CD103 + dDCs and, to the best of our knowledge, the study presented herein is the first to do so.…”

Section: Discussionmentioning

confidence: 98%

Subcutaneous cholera toxin exposure induces potent CD103⁺ dermal dendritic cell activation and migration

et al. 2013

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CD103 + dermal dendritic cells (dDCs) are a recently described DC subset of the skin shown to be the principal migratory DCs capable of efficiently cross-presenting antigens and activating CD8 + T cells. Harnessing their activity would promote vaccine efficacy, but it has been unclear how this can be achieved. We tested a panel of adjuvants for their ability to affect dDCs. In comparison to the other adjuvants tested, the capacity of cholera toxin (CT) to induce the migration of dDCs was unique. Within 24 h of CT injection, large numbers of highly activated dDCs (including CD103 + dDCs) migrated to the draining lymph nodes and cross-presented coinjected antigens, potently activating naïve CD8 + T cells. Peptide vaccines adjuvanted with CT induced T-cell responses uniquely characterized by dynamic cytokine responses including the production of IL-2, and such vaccines were protective in situations reliant on CD8 + T-cell responses, including liver-stage Plasmodium challenge, or tumor challenge. This study is the first to examine the effects of adjuvants on CD103 + dDCs and identifies CT as a prototypical adjuvant for the activation of CD103 + dDCs, opening the way to development of vaccines and adjuvants that specifically target dDCs and generate effective CD8 + T-cell responses.

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Section: Discussionmentioning

confidence: 98%

Subcutaneous cholera toxin exposure induces potent CD103⁺ dermal dendritic cell activation and migration

et al. 2013

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“…Exchange of membrane molecules/ Ags between immune cells has been observed for a long time (4,5), but the mechanisms and functional consequences of these transfers have not been completely elucidated. Nevertheless, several studies (3,(6)(7)(8)(9) reported that transfer of peptide-MHC complexes on DCs is a potential additional mechanism for activating T cells and referred to the process as "DC cross-dressing," a term originally coined by Yewdell and Haeryfar (10). Although cross-dressing has been clearly shown in conventional myeloid DCs (mDCs), this phenomenon has never been reported in plasmacytoid DCs (pDCs).…”

Section: O Ptimal Activation Of Tumor-specific Cytotoxic Cd8 + T Celmentioning

confidence: 99%

Membrane Transfer from Tumor Cells Overcomes Deficient Phagocytic Ability of Plasmacytoid Dendritic Cells for the Acquisition and Presentation of Tumor Antigens

Bonaccorsi

Morandi

Antsiferova

et al. 2014

The Journal of Immunology

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The potential contribution of plasmacytoid dendritic cells (pDCs) in the presentation of tumor cell Ags remains unclear, and some controversies exist with regard to the ability of pDCs to phagocytose cell-derived particulate Ags and cross-present them to MHC class I–restricted T lymphocytes. In this study, we show that human pDCs, although inefficient in the internalization of cell membrane fragments by phagocytosis, can efficiently acquire membrane patches and associated molecules from cancer cells of different histotypes. The transfer of membrane patches to pDCs occurred in a very short time and required cell-to-cell contact. Membrane transfer also included intact HLA complexes, and the acquired Ags could be efficiently recognized on pDCs by tumor-specific CD8+ T cells. Remarkably, pDCs isolated from human colon cancer tissues displayed a strong surface expression of epithelial cell adhesion molecule, indicating that the exchange of exogenous Ags between pDCs and tumor cells also can occur in vivo. These data demonstrate that pDCs are well suited to acquire membrane patches from contiguous tumor cells by a cell-to-cell contact–dependent mechanism that closely resembles “trogocytosis.” This phenomenon may allow pDCs to proficiently present tumor cell–derived Ags, despite limited properties of endophagocytosis.

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“…This fusion protein, whose N-terminal part lacks a defined tertiary structure, does feed well into the MHC class I antigen processing machinery of the cell expressing it endogenously, but does not give rise to substantial levels of stable protein, that is, no detectable GFP expression, and thus likely represents a very poor substrate for crosspresentation (Probst et al, 2003). The absence of priming by DCs that do not carry the DIETER transgene itself (Muth et al, 2014) also rules out functionally relevant DC-to-DC antigen transfer by means other than cross-presentation, such as the transfer of fully assembled peptide/MHC complexes by trogocytosis that has been dubbed "cross dressing" (Dolan et al, 2006;Li et al, 2012).…”

Section: Discussionmentioning

confidence: 99%

Dermal CD207-Negative Migratory Dendritic Cells Are Fully Competent to Prime Protective, Skin Homing Cytotoxic T-Lymphocyte Responses

Hain

Melchior

Kamenjarin

et al. 2019

Journal of Investigative Dermatology

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Dendritic cells (DCs) are important inducers and regulators of T-cell responses. They are able to activate and modulate the differentiation of CD4 þ and CD8 þ T cells. In the skin, there are at least five phenotypically distinct DC subpopulations that can be distinguished by differential expression of the cell surface markers CD207, CD103, and CD11b. Previous studies have suggested that dermal CD11b À CD207 þ conventional type 1 DCs are indispensable for the priming of a skin homing cytotoxic T-lymphocyte response. However, conventional type 1 DCs are also the only skin DC subset capable of cross-presenting exogenous antigens on major histocompatibility complex class I. Thus, it remained unclear whether for antigens that do not require crosspresentation, such as viruses that infect DCs, other DC subtypes in the skin can contribute to cytotoxic T-lymphocyte priming. To address this question, we used a transgenic mouse model that allows inducible expression and presentation of a model antigen on selected subsets of dermal DCs. We show that for antigens presented via the conventional major histocompatibility complex class I presentation pathway, CD207 e dermal DCs are fully competent to prime a skin homing cytotoxic T-lymphocyte response that is capable of protection against a local virus challenge and gives rise to skin resident memory CD8 þ T cells.

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Cross-dressed CD8α ⁺ /CD103 ⁺ dendritic cells prime CD8 ⁺ T cells following vaccination

Cited by 63 publications

References 21 publications

Subcutaneous cholera toxin exposure induces potent CD103⁺ dermal dendritic cell activation and migration

Subcutaneous cholera toxin exposure induces potent CD103⁺ dermal dendritic cell activation and migration

Membrane Transfer from Tumor Cells Overcomes Deficient Phagocytic Ability of Plasmacytoid Dendritic Cells for the Acquisition and Presentation of Tumor Antigens

Dermal CD207-Negative Migratory Dendritic Cells Are Fully Competent to Prime Protective, Skin Homing Cytotoxic T-Lymphocyte Responses

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Cross-dressed CD8α + /CD103 + dendritic cells prime CD8 + T cells following vaccination

Cited by 63 publications

References 21 publications

Subcutaneous cholera toxin exposure induces potent CD103+ dermal dendritic cell activation and migration

Subcutaneous cholera toxin exposure induces potent CD103+ dermal dendritic cell activation and migration

Membrane Transfer from Tumor Cells Overcomes Deficient Phagocytic Ability of Plasmacytoid Dendritic Cells for the Acquisition and Presentation of Tumor Antigens

Dermal CD207-Negative Migratory Dendritic Cells Are Fully Competent to Prime Protective, Skin Homing Cytotoxic T-Lymphocyte Responses

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About

Cross-dressed CD8α ⁺ /CD103 ⁺ dendritic cells prime CD8 ⁺ T cells following vaccination

Subcutaneous cholera toxin exposure induces potent CD103⁺ dermal dendritic cell activation and migration

Subcutaneous cholera toxin exposure induces potent CD103⁺ dermal dendritic cell activation and migration