Langerhans cells and viral immunity

Cunningham, Anthony L.; Carbone, Federico; Geijtenbeek, Teunis B. H.

doi:10.1002/eji.200838521

Cited by 55 publications

(45 citation statements)

References 88 publications

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“…Recent evidence suggests that langerin 2 dDCs and langerin + dDCs are the cutaneous DC subsets that present viral Ag to naive T cells postinfection of murine skin (22,41). LCs are the major APCs in the epidermis and so are likely to be the first DC subset to encounter HSV, because this infection is first confined to the epidermis, but their role in the immune response to acute HSV skin infection remains unclear.…”

Section: Discussionmentioning

confidence: 99%

Herpes Simplex Virus Infects Skin γδ T Cells before Langerhans Cells and Impedes Migration of Infected Langerhans Cells by Inducing Apoptosis and Blocking E-Cadherin Downregulation

Puttur

Fernandez

White

et al. 2010

The Journal of Immunology

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The role individual skin dendritic cell (DC) subsets play in the immune response to HSV remains unclear. We investigated the effect of HSV on DC virus uptake, viability, and migration after cutaneous infection in vitro and in vivo. HSV increased the emigration of skin DCs from whole skin explants over 3 d postinfection (p.i.) compared with mock controls, but the kinetics of emigration was influenced by the skin DC subset. Uninfected (bystander) Langerhans cells (LCs) were the major emigrant DC subset at 24 h p.i., but thereafter, large increases in infected CD103+langerin+ dermal DC (dDC) and uninfected langerin− dDC emigration were also observed. LC infection was confirmed by the presence of HSV glycoprotein D (gD) and was associated with impaired migration from cultured skin. Langerin+ dDC also expressed HSV gD, but infection did not impede migration. We then followed the virus in live MacGreen mice in which LCs express GFP using a fluorescent HSV-1 strain by time-lapse confocal microscopy. We observed a sequential infection of epidermal cells, first in keratinocytes and epidermal γδ T cells at 6 h p.i., followed by the occurrence of HSVgD+ LCs at 24 h p.i. HSV induced CCR7 upregulation on all langerin+ DC, including infected LCs, and increased production of skin TNF-α and IL-1β. However, a large proportion of infected LCs that remained within the skin was apoptotic and failed to downregulate E-cadherin compared with bystander LCs or mock controls. Thus, HSV infection of LCs is preceded by infection of γδ T cells and delays migration.

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Section: Discussionmentioning

confidence: 99%

Herpes Simplex Virus Infects Skin γδ T Cells before Langerhans Cells and Impedes Migration of Infected Langerhans Cells by Inducing Apoptosis and Blocking E-Cadherin Downregulation

Puttur

Fernandez

White

et al. 2010

The Journal of Immunology

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“…Upon infection of the mucosal tissues, HSV encounters a variety of cells, including dendritic cells (DCs), that bridge innate and adaptive immunity (7). Immature DCs are able to capture and process viral antigens.…”

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confidence: 99%

A Herpesvirus Virulence Factor Inhibits Dendritic Cell Maturation through Protein Phosphatase 1 and IκB Kinase

Jin

Yan

et al. 2011

J Virol

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Dendritic cells are sentinels in innate and adaptive immunity. Upon virus infection, a complex program is in operation, which activates IB kinase (IKK), a key regulator of inflammatory cytokines and costimulatory molecules. Here we show that the ␥ 1 34.5 protein, a virulence factor of herpes simplex viruses, blocks Toll-like receptor-mediated dendritic cell maturation. While the wild-type virus inhibits the induction of major histocompatibility complex (MHC) class II, CD86, interleukin-6 (IL-6), and IL-12, the ␥ 1 34.5-null mutant does not. Notably, ␥ 1 34.5 works in the absence of any other viral proteins. When expressed in mammalian cells, including dendritic cells, ␥ 1 34.5 associates with IKK␣/␤ and inhibits NF-B activation. This is mirrored by the inhibition of IKK␣/␤ phosphorylation, p65/RelA phosphorylation, and nuclear translocation in response to lipopolysaccharide or poly(I:C) stimulation. Importantly, ␥ 1 34.5 recruits both IKK␣/␤ and protein phosphatase 1, forming a complex that dephosphorylates two serine residues within the catalytic domains of IB kinase. The amino-terminal domain of ␥ 1 34.5 interacts with IKK␣/␤, whereas the carboxyl-terminal domain binds to protein phosphatase 1. Deletions or mutations in either domain abolish the activity of ␥ 1 34.5. These results suggest that the control of IB kinase dephosphorylation by ␥ 1 34.5 represents a critical viral mechanism to disrupt dendritic cell functions.Herpes simplex virus 1 (HSV-1), a member of the Herpesviridae, establishes both latent and lytic infection (45). Upon infection of the mucosal tissues, HSV encounters a variety of cells, including dendritic cells (DCs), that bridge innate and adaptive immunity (7). Immature DCs are able to capture and process viral antigens. When activated, DCs express a high level of costimulatory molecules. Moreover, DCs release inflammatory cytokines to promote DC maturation. A prominent feature of DCs is to activate naive T cells, where myeloid mucosal and lymph node-resident DCs are responsible for HSV-specific T cell activation (1,40,47).A complex program is in operation upon DC maturation, which is coupled to Toll-like receptor (TLR)-related pathways (34). For example, when exposed to lipopolysaccharide (LPS) or viral proteins (3, 24, 41), TLR4 activates the two arms of downstream signaling. In this process, TLR4 recruits TRIF via an adaptor, TRAM, and migrates to the endosomal membrane, where it activates TANK binding kinase 1 (TBK1) and interferon (IFN) regulatory factor 3 (IRF3). In parallel, TLR4 engages with MyD88 through the adaptor TIRAP (also called Mal) at the plasma membrane, which facilitates the formation of a complex consisting of TRAF6, TAK1, TAB2, and IRAK. This relays signals to IB kinase (IKK), containing the IKK␣, ⌱⌲⌲␤, and IKK␥ subunits. Activated IB kinase phosphorylates IB proteins to trigger their ubiquitination and proteosome-mediated degradation, leading to the nuclear translocation of NF-B, which usually exists as a p65 (RelA)/p50 heterodimer (12). Accordingly, TLR activation upr...

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“…In the skin, LCs are the obvious primary DC subset likely to be initially involved in HSV-1 antigen uptake, and, accordingly, earlier analyses on the role of LCs in anti-HSV-1 immunity claimed that depletion of LCs before infection leads to increased HSV-1 virulence (Sprecher and Becker, 1986). However, more recently, several studies have conclusively shown that in WT mice, LCs are not the cells presenting HSV-1 antigens to CD8 + T cells and thus are not directly involved in the induction of MHC class I-restricted antiviral immune responses (Allan et al, 2006;Cunningham et al, 2008;Bedoui et al, 2009;Eidsmo et al, 2009;Puttur et al, 2010). After epicutaneous HSV-1 infection, lymph noderesident CD8α + DCs or migratory CD103 + dermal DCs were identified to be the predominant DC population presenting HSV-1 antigens to CD8 + T cells (Allan et al, 2006;Bedoui et al, 2009).…”

Section: Discussionmentioning

confidence: 96%

“…Interestingly, although LCs are the primary cutaneous antigen-acquiring cells it has been shown that lymph node-resident DCs but not LCs induce MHC class I-restricted antiviral immunity and the priming of HSV-1-specific CTLs (Allan et al, 2003;Cunningham et al, 2008;Bedoui et al, 2009), most likely because HSV-1-infected LCs appeared to be compromised in their trafficking ability as they failed to downregulate E-cadherin or undergo apoptosis after HSV-1 infection (Bosnjak et al, 2005;Eidsmo et al, 2009;Cunningham et al, 2010;Puttur et al, 2010).…”

Section: Introductionmentioning

confidence: 97%

Cutaneous RANK–RANKL Signaling Upregulates CD8-Mediated Antiviral Immunity during Herpes simplex Virus Infection by Preventing Virus-Induced Langerhans Cell Apoptosis

Klenner

Hafezi

Clausen³

et al. 2015

Journal of Investigative Dermatology

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Herpes simplex virus-type 1 (HSV-1) causes the majority of cutaneous viral infections. Viral infections are controlled by the immune system, and CD8(+) cytotoxic T-lymphocytes (CTLs) have been shown to be crucial during the clearance of HSV-1 infections. Although epidermal Langerhans cells (LCs) are the first dendritic cells (DCs) to come into contact with the virus, it has been shown that the processing of viral antigens and the differentiation of antiviral CTLs are mediated by migratory CD103(+) dermal DCs and CD8α(+) lymph node-resident DCs. In vivo regulatory T-cells (Tregs) are implicated in the regulation of antiviral immunity and we have shown that signaling via the receptor activator of NF-κB (RANK) and its ligand RANKL mediates the peripheral expansion of Tregs. However, in addition to expanding Tregs, RANK-RANKL interactions are involved in the control of antimicrobial immunity by upregulating the priming of CD4(+) effector T cells in LCMV infection or by the generation of parasite-specific CD8(+) T cells in Trypanosoma cruzi infection. Here, we demonstrate that cutaneous RANK-RANKL signaling is critical for the induction of CD8-mediated antiviral immune responses during HSV-1 infection of the skin by preventing virus-induced LC apoptosis, improving antigen transport to regional lymph nodes, and increasing the CTL priming capacity of lymph node DCs.

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Langerhans cells and viral immunity

Cited by 55 publications

References 88 publications

Herpes Simplex Virus Infects Skin γδ T Cells before Langerhans Cells and Impedes Migration of Infected Langerhans Cells by Inducing Apoptosis and Blocking E-Cadherin Downregulation

Herpes Simplex Virus Infects Skin γδ T Cells before Langerhans Cells and Impedes Migration of Infected Langerhans Cells by Inducing Apoptosis and Blocking E-Cadherin Downregulation

A Herpesvirus Virulence Factor Inhibits Dendritic Cell Maturation through Protein Phosphatase 1 and IκB Kinase

Cutaneous RANK–RANKL Signaling Upregulates CD8-Mediated Antiviral Immunity during Herpes simplex Virus Infection by Preventing Virus-Induced Langerhans Cell Apoptosis

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