Poxvirus Infection-Associated Downregulation of C-Type Lectin-Related-b Prevents NK Cell Inhibition by NK Receptor Protein-1B

Williams, Kibileri; Wilson, Evan; Davidson, Courtney; Aguilar, Oscar A.; Fu, Li; Carlyle, James R.; Burshtyn, Deborah N.

doi:10.4049/jimmunol.1103425

Cited by 33 publications

(36 citation statements)

References 58 publications

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“…In agreement with this, similar findings were reported for mClr-b in a mouse model of orthopoxvirus (VV, ECTV) infection [15] . Here, we provide evidence for a conserved mechanistic response for both mClr-b and rClr-11 in response to cross-species CMV infection.…”

Section: Discussionsupporting

confidence: 80%

“…We next tested the effects of the proteasomal inhibitor, MG132, on MCMV infection-mediated Clr-b loss, as we previously showed that inhibition of the Ub-proteasome degradation pathway could prevent genotoxic stressmediated Clr-b downregulation [14,15] . MG132 was effective at blocking MCMV-mediated Clr-b loss, albeit incompletely even at high doses (online suppl.…”

Section: Mcmv-mediated Mclr-b Downregulation Is Partially Blocked By mentioning

confidence: 99%

“…fig. 2) or that ActD may also promote stress-mediated mClr-b downregulation [14,15] . Thus, we attempted to titrate ActD levels to achieve only partial Clr-b loss, while maintaining partial inhibition of IE genes; however, such an optimal dose was not possible, making inferences on IE gene blockade inconclusive (online suppl.…”

Section: Mcmv-mediated Mclr-b Downregulation Is Partially Blocked By mentioning

confidence: 99%

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Modulation of Clr Ligand Expression and NKR-P1 Receptor Function during Murine Cytomegalovirus Infection

Aguilar

Mesci²,

Ma³

et al. 2015

J Innate Immun

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Viruses are known to induce pathological cellular states that render infected cells susceptible or resistant to immune recognition. Here, we characterize an MHC-I-independent natural killer (NK) cell recognition mechanism that involves modulation of inhibitory NKR-P1B:Clr-b receptor-ligand interactions in response to mouse cytomegalovirus (MCMV) infection. We demonstrate that mouse Clr-b expression on healthy cells is rapidly lost at the cell surface and transcript levels in a time- and dose-dependent manner upon MCMV infection. In addition, cross-species infections using rat cytomegalovirus (RCMV) infection of mouse fibroblasts and MCMV infection of rat fibroblasts suggest that this response is conserved during host-pathogen interactions. Active viral infection appears to be necessary for Clr-b loss, as cellular stimulation using UV-inactivated whole virus or agonists of many innate pattern recognition receptors failed to elicit efficient Clr-b downregulation. Notably, Clr-b loss could be partially blocked by titrated cycloheximide treatment, suggesting that early viral or nascent host proteins are required for Clr-b downregulation. Interestingly, reporter cell assays suggest that MCMV may encode a novel Clr-b-independent immunoevasin that functionally engages the NKR-P1B receptor. Together, these data suggest that Clr-b modulation is a conserved innate host cell response to virus infection that is subverted by multiple CMV immune evasion strategies.

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Section: Discussionsupporting

confidence: 80%

Section: Mcmv-mediated Mclr-b Downregulation Is Partially Blocked By mentioning

confidence: 99%

Section: Mcmv-mediated Mclr-b Downregulation Is Partially Blocked By mentioning

confidence: 99%

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Modulation of Clr Ligand Expression and NKR-P1 Receptor Function during Murine Cytomegalovirus Infection

Aguilar

Mesci²,

Ma³

et al. 2015

J Innate Immun

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“…The murine NKR-P1B ligand, , is rapidly lost in response to cellular infection by diverse viruses Voigt et al, 2007;Williams et al, 2012). However, MCMV-infected fibroblasts also induce a Clr-b-independent NKR-P1B ligand .…”

Section: Encodes An Nkr-p1b Decoy Immunoevasinmentioning

confidence: 99%

“…Yet to date, NKR-P1C, the prototypical NK1.1 antigen in B6 mice (Glimcher et al, 1977;Koo and Peppard, 1984;Ryan et al, 1992), and NKR-P1A remain orphan-activating receptors with unknown physiological ligands. On the other hand, the paired NKR-P1F and NKR-P1G receptors recognize overlapping ''self'' Clr (Clec2) ligands to balance signals during NK cell education and effector responses, while the inhibitory NKR-P1B receptor recognizes the broadly expressed self Clr-b (Clec2d) ligand (Carlyle et al, 2004;Chen et al, 2011;Iizuka et al, 2003;Kveberg et al, 2009 been shown to be involved in ''missing-self'' recognition under diverse pathological states (Kirkham and Carlyle, 2014), including cancer (Carlyle et al, 2004), genotoxic and cellular stress (Fine et al, 2010), hematopoietic transplantation , immune escape of primary lymphoma cells , and cytomegalovirus and poxvirus infection Voigt et al, 2007;Williams et al, 2012), while the remainder of the self Clr ligands remain less well characterized. Among pathogens recognized by NK cells, cytomegaloviruses (CMV) demonstrate co-evolution with their natural hosts, likely due to cycles of natural selection for viral versus host fitness.…”

Section: Natural Killer (Nk) Cells Are a Subset Of Innate Lymphoid Cementioning

confidence: 99%

A Viral Immunoevasin Controls Innate Immunity by Targeting the Prototypical Natural Killer Cell Receptor Family

Aguilar

Berry

Rahim

et al. 2017

Cell

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The evolutionary arms race between NK cells and viruses: Who gets the short end of the stick?

2013

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NK cells in viral infectionsNK cells are innate cytotoxic lymphocytes essential for the control of a broad range of viral infections. The activation and function of NK cells are based on a tightly regulated interplay between inhibitory and activating signals induced by the receptors expressed on their surface (reviewed in [1]) or by a variety of cytokines generated by the interaction between NK cells and other innate immune cells, such as macrophages and DCs [2,3]. Type I IFNs, IL-12, IL-15, and IL-18 produced by macrophages and DCs are indispensable for NK-cell maturation and regulation of NK-cell function. More recently, it has been demonstrated that TGF-β signaling limits the maturation dynamics of NK cells during the neonatal period [4]. Mice lacking the TGF-β receptor on the surface of their NK cells and DCs possess more mature NK cells and can therefore control viral infection more efficiently compared with control mice [4], providing an explanation for the deficient NK-cell response early in life.Correspondence: Prof. Stipan Jonjić e-mail: stipan.jonjic@medri.uniri.hrThe impact of NK cells on virus control has been proven to play a key role in different infection models including those modeling infection with influenza virus, HIV, HCV, coxsackievirus, and poxviruses. Arguably, the role of NK cells in the control of herpesviruses, especially CMV, has been most widely studied up till now (reviewed in [5][6][7]). Upon activation and recruitment to the site of infection, NK cells use several mechanisms to limit virus replication: (i) a cytolytic response involving the secretion of cytolytic granules (granzymes and perforin) upon engagement of an activating receptor [8,9], (ii) production of pro-inflammatory cytokines with antiviral activity such as , (iii) killing of target cells via FasL or TRAIL [11], and (iv) Abdependent, cell-mediated cytotoxicity-mediated lysis via CD16 [12].Besides their well-recognized role in the control of virus replication, NK cells have been shown to possess additional functions that can be beneficial or detrimental to the host. For instance, decidual NK cells are considered to be important for placentation and maintenance of materno-fetal immune tolerance [13], but there is a very limited amount of data published on the role of NK cells in the control of infections during pregnancy. In mouse cytomegalovirus (MCMV)-infected mice, NK cells preserve the integrity and function of the salivary gland, an organ that iswww.eji-journal.eu 868Antonija Miletić et al. Eur. J. Immunol. 2013. 43: 867-877 important for horizontal virus spread [14,15]. A study using the mouse model of salivary gland dysfunction after an acute MCMV infection showed the involvement of NK cells in the prevention of acinar atrophy and loss of secretions [16]. Conversely, the NK-cell response could play a negative role in virus infection, as demonstrated in the case of infection with RSV [17]. NK cells accumulate in the lungs of BALB/c mice at the early stage of RSV infection, where they gain an activated phenotyp...

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Poxvirus Infection-Associated Downregulation of C-Type Lectin-Related-b Prevents NK Cell Inhibition by NK Receptor Protein-1B

Cited by 33 publications

References 58 publications

Modulation of Clr Ligand Expression and NKR-P1 Receptor Function during Murine Cytomegalovirus Infection

Modulation of Clr Ligand Expression and NKR-P1 Receptor Function during Murine Cytomegalovirus Infection

A Viral Immunoevasin Controls Innate Immunity by Targeting the Prototypical Natural Killer Cell Receptor Family

The evolutionary arms race between NK cells and viruses: Who gets the short end of the stick?

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