CD8α2 CD11b+ Dendritic Cells Present Exogenous Virus-like Particles to CD8+ T Cells and Subsequently Express CD8α and CD205 Molecules

Morón, Gabriel; Rueda, Paloma; Casal, J. Ignacio; Leclerc, Claude

doi:10.1084/jem.20011930

Cited by 117 publications

(94 citation statements)

References 57 publications

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“…Martinez del Hoyo et al reported that splenic CD8a -DC differentiate into CD8a + DC in vivo [30], although another recent study presented conflicting results [31]. Moreover, several recent studies indicate that the surface expression level of CD11b on CD8a + and CD8a -DC subsets changes during maturation or after Ag uptake, at least in the spleen [32,33]. In this study, we could not determine whether DC underwent phenotypic change after OVA uptake, because we isolated DC at a single time point after OVA administration.…”

Section: Discussionmentioning

confidence: 99%

Anatomic location defines antigen presentation by dendritic cells to T cells in response to intravenous soluble antigens

Chung¹,

Chang²,

Kim³

et al. 2007

Eur J Immunol

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In the spleen, exogenous antigen is preferentially presented by CD8a + CD11b -DC to CD8 T cells and by CD8a -CD11b + DC to CD4 T cells. However, it is not yet clear whether the same rule applies to other secondary lymphoid organs. To address this issue, we first classified secondary lymphoid tissues into three categories based on the expression pattern of CD8a and CD11b in C57BL/6 and BALB/c mice: (a) spleen, (b) mesenteric lymph node (MLN) and (c) other peripheral lymph nodes (PLN). We then analyzed the OVA-specific T cell-stimulating capacity of each DC subset after intravenous injection with soluble OVA. Our results show that, regardless of tissue origin, CD8a -CD11b + DC generally present OVA to CD4 T cells, a finding that held true as well for CD8a + CD11b + DC in PLN. In striking contrast, CD8a + CD11b -DC in spleen, CD8a -CD11b + DC in MLN and CD8a + CD11b + DC in PLN mainly cross-present OVA to CD8 T cells in their respective tissues. Of note, CD8a -CD11b + DC in MLN and CD8a + CD11b + DC in PLN present OVA to both CD4 T and CD8 T cells. Therefore, the antigen-presenting capacity of each distinct DC subset is determined by its anatomic environment in combination with its surface phenotype.

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Section: Discussionmentioning

confidence: 99%

Anatomic location defines antigen presentation by dendritic cells to T cells in response to intravenous soluble antigens

Chung¹,

Chang²,

Kim³

et al. 2007

Eur J Immunol

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“…Although originally the expression of CD8␣ was used to mark DCs thought to be of lymphoid origin (1,34), it is now clear that this surface Ag is expressed on a variety of quite different DC subsets. We were interested in two particular subsets expressing CD8 that have been implicated in either CTL priming (12,13,35) or antiviral immunity (5,14). The first is the conventional CD8 DC subset identified by Vremec et al (1) and which has recently been shown to be important in cross-presentation of Ag for both CTL priming and tolerance (12,29).…”

Section: Resultsmentioning

confidence: 99%

“…These DCs have been shown to preferentially cross-present model cell-associated Ags to prime CD8 ϩ T cell responses, consistent with the notion that they play a key role in generating antiviral immunity (12). However, while this subset has been shown to preferentially present class I-restricted Ag derived from nonreplicating virus-like particles (13), there is currently no comparable data involving an infectious live virus. In addition, other DC subsets have been implicated in other aspects of antiviral immunity.…”

mentioning

confidence: 87%

Cutting Edge: Conventional CD8α+ Dendritic Cells Are Preferentially Involved in CTL Priming After Footpad Infection with Herpes Simplex Virus-1

Smith¹,

Belz

Wilson³

et al. 2003

The Journal of Immunology

167

168

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CTL play a major role in immunity to HSV type 1, but little is known about the priming process. In this study, we have examined the class I-restricted presentation of an immunodominant determinant from HSV-1 glycoprotein B after footpad infection. We have found that the only cell types capable of presenting this determinant in draining popliteal lymph nodes within the first 3 days after infection are the CD11c+CD8α+CD45RA− dendritic cells. Given that such class I-restricted presentation is essential for CTL priming, this implies that these conventional CD8α+ dendritic cells are the key subset involved in CTL immunity to this virus.

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“…Indeed, an lymphocytic choriomeningitis virus infection has been shown to change the predominant DC subset from pDC to mDC to divert host immune response away from anti-viral immunity [24]. On the other hand, it was reported that pDC accumulate in the spleen after infection with murine cytomegalovirus [25], and that mDC present exogenous virus-like particles to CD8 T cells and subsequently become CD8 + [26].…”

Section: Introductionmentioning

confidence: 99%

Vaccinia virus infection induces dendritic cell maturation but inhibits antigen presentation by MHC class II

Yao

Singh

et al. 2007

Cellular Immunology

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Vaccinia virus (VV) infection is known to inhibit dendritic cells (DC) functions in vitro.Paradoxically, VV is also highly immunogenic and thus has been used as a vaccine. In the present study, we investigated the effects of an in vivo VV infection on DC function by focusing on early innate immunity. Our data indicated that DC are activated upon in vivo VV infection of mice. Splenic DC from VV-infected mice expressed elevated levels of MHC class I and co-stimulatory molecules on their cell surface and exhibited the enhanced potential to produce cytokines upon LPS stimulation. DC from VV-infected mice also expressed a high level of interferon-β. However, a VV infection resulted in the down-regulation of MHC class II expression and the impairment of antigen presentation to CD4 T cells by DC. Thus, during the early stage of a VV infection, although DC are impaired in some of the critical antigen presentation functions, they can promote innate immune defenses against viral infection.

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CD8α2 CD11b+ Dendritic Cells Present Exogenous Virus-like Particles to CD8+ T Cells and Subsequently Express CD8α and CD205 Molecules

Cited by 117 publications

References 57 publications

Anatomic location defines antigen presentation by dendritic cells to T cells in response to intravenous soluble antigens

Anatomic location defines antigen presentation by dendritic cells to T cells in response to intravenous soluble antigens

Cutting Edge: Conventional CD8α+ Dendritic Cells Are Preferentially Involved in CTL Priming After Footpad Infection with Herpes Simplex Virus-1

Vaccinia virus infection induces dendritic cell maturation but inhibits antigen presentation by MHC class II

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