Your search keyword '"Iyer, Ravi F."' showing total 5 results

1. Human cytomegalovirus UL18 prevents priming of MHC-E– and MHC-II–restricted CD8+ T cells.

Author

Malouli, Daniel, Taher, Husam, Mansouri, Mandana, Iyer, Ravi F., Reed, Jason, Papen, Courtney, Schell, John B., Beechwood, Teresa, Martinson, Thomas, Morrow, David, Hughes, Colette M., Gilbride, Roxanne M., Randall, Kurt, Ford, Julia C., Belica, Karina, Ojha, Sohita, Sacha, Jonah B., Bimber, Benjamin N., Hansen, Scott G., and Picker, Louis J.

Subjects

T cell receptors, SIMIAN immunodeficiency virus, T cells, MAJOR histocompatibility complex, GENETIC vectors

Abstract

Rhesus cytomegalovirus (RhCMV) vectors elicit major histocompatibility complex (MHC)–E–restricted CD8+ T cells that stringently control simian immunodeficiency virus (SIV) in rhesus macaques. These responses require deletion of eight RhCMV chemokine-like open reading frames (ORFs) that are conserved in human cytomegalovirus (HCMV). To determine whether HCMV encodes additional, nonconserved inhibitors of unconventional T cell priming, we inserted 41 HCMV-specific ORFs into a chemokine-deficient strain (68-1 RhCMV). Monitoring of epitope recognition revealed that HCMV UL18 prevented unconventional T cell priming, resulting in MHC-Ia–targeted responses. UL18 is homologous to MHC-I but does not engage T cell receptors and, instead, binds with high affinity to inhibitory leukocyte immunoglobulin-like receptor–1 (LIR-1). UL18 lacking LIR-1 binding no longer interfered with MHC-E–restricted T cell stimulation by RhCMV-infected cells or the induction of unconventionally restricted T cells. Thus, LIR-1 binding needs to be deleted from UL18 of HCMV/HIV vaccines to allow for the induction of protective MHC-E–restricted T cells. Editor's summary: Rhesus cytomegalovirus (RhCMV)–based vectors expressing simian immunodeficiency virus (SIV) antigens can control SIV in rhesus macaques by inducing major histocompatibility complex (MHC)–E–restricted CD8 T cells, but this response requires deletion of eight RhCMV chemokine-like open reading frames (ORFs) that are conserved in human cytomegalovirus (HCMV). Toward optimizing HCMV-based viral vectors, Malouli et al. screened 41 HCMV-specific ORFs and observed that strain 68-1 RhCMV expressing HCMV UL18 vector elicited MHC-Ia–restricted T cells despite being chemokine deficient. UL18 has homology to MHC-I and binds to inhibitory leukocyte immunoglobulin-like receptor–1 (LIR-1) but not T cell receptors. Disruption of UL18 binding to LIR-1 is sufficient to permit MHC-E–restricted T cell activation, thus suggesting that deletion of UL18 in HCMV-based HIV vectors may enhance induction of protective immunity. —Christiana Fogg [ABSTRACT FROM AUTHOR]

Published

2024

2. The secreted protein Cowpox Virus 14 contributes to viral virulence and immune evasion by engaging Fc-gamma-receptors.

Author

Iyer, Ravi F., Edwards, David M., Kolb, Philipp, Raué, Hans-Peter, Nelson, Chris A., Epperson, Megan L., Slifka, Mark K., Nolz, Jeffrey C., Hengel, Hartmut, Fremont, Daved H., and Früh, Klaus

Subjects

*VIRAL proteins, *VACCINIA, *ANTIGEN presentation, *FC receptors, *T cells, *IMMUNOMODULATORS, *RECEPTOR antibodies

Abstract

The genome of cowpoxvirus (CPXV) could be considered prototypical for orthopoxviridae (OXPV) since it contains many open reading frames (ORFs) absent or lost in other OPXV, including vaccinia virus (VACV). These additional ORFs are non-essential for growth in vitro but are expected to contribute to the broad host range, virulence and immune evasion characteristics of CPXV. For instance, unlike VACV, CPXV encodes proteins that interfere with T cell stimulation, either directly or by preventing antigen presentation or co-stimulation. When studying the priming of naïve T cells, we discovered that CPXV, but not VACV, encodes a secreted factor that interferes with activation and proliferation of naïve CD8+ and CD4+ T cells, respectively, in response to anti-CD3 antibodies, but not to other stimuli. Deletion mapping revealed that the inhibitory protein is encoded by CPXV14, a small secreted glycoprotein belonging to the poxvirus immune evasion (PIE) family and containing a smallpoxvirus encoded chemokine receptor (SECRET) domain that mediates binding to chemokines. We demonstrate that CPXV14 inhibition of antibody-mediated T cell activation depends on the presence of Fc-gamma receptors (FcγRs) on bystander cells. In vitro, CPXV14 inhibits FcγR-activation by antigen/antibody complexes by binding to FcγRs with high affinity and immobilized CPXV14 can trigger signaling through FcγRs, particularly the inhibitory FcγRIIB. In vivo, CPXV14-deleted virus showed reduced viremia and virulence resulting in reduced weight loss and death compared to wildtype virus whereas both antibody and CD8+ T cell responses were increased in the absence of CPXV14. Furthermore, no impact of CPXV14-deletion on virulence was observed in mice lacking the inhibitory FcγRIIB. Taken together our results suggest that CPXV14 contributes to virulence and immune evasion by binding to host FcγRs. Author summary: Coxpoxvirus is considered the prototypical member of the closely related orthopox virus family that includes monkeypoxvirus and Variola major which caused smallpox. Presumably due to the presence of a large number of ORFs encoding for immunomodulators, CPXV is capable of infecting a wide variety of host species. Here, we show that the ORF CPXV14 encodes a small secreted protein that binds to host receptors for the constant Fc region of IgG antibodies thus preventing the ability of antibodies to engage these receptors. Viruses lacking CPXV14 are less virulent in animals but elicit increased immune responses suggesting that the interference with antibody function contributes to the ability of CPXV to evade immune control. Targeting Fc receptors is thus a new type of immune evasion mechanism that has possible applications for antibody mediated therapies. [ABSTRACT FROM AUTHOR]

Published

2022

3. Human cytomegalovirus UL18 prevents priming of MHC-E- and MHC-II-restricted CD8 + T cells.

Author

Malouli D, Taher H, Mansouri M, Iyer RF, Reed J, Papen C, Schell JB, Beechwood T, Martinson T, Morrow D, Hughes CM, Gilbride RM, Randall K, Ford JC, Belica K, Ojha S, Sacha JB, Bimber BN, Hansen SG, Picker LJ, and Früh K

Subjects

Animals, Humans, Viral Proteins immunology, Histocompatibility Antigens Class II immunology, Histocompatibility Antigens Class I immunology, Cytomegalovirus Infections immunology, Cytomegalovirus Infections prevention & control, CD8-Positive T-Lymphocytes immunology, Cytomegalovirus immunology, Macaca mulatta

Abstract

Rhesus cytomegalovirus (RhCMV) vectors elicit major histocompatibility complex (MHC)-E-restricted CD8 + T cells that stringently control simian immunodeficiency virus (SIV) in rhesus macaques. These responses require deletion of eight RhCMV chemokine-like open reading frames (ORFs) that are conserved in human cytomegalovirus (HCMV). To determine whether HCMV encodes additional, nonconserved inhibitors of unconventional T cell priming, we inserted 41 HCMV-specific ORFs into a chemokine-deficient strain (68-1 RhCMV). Monitoring of epitope recognition revealed that HCMV UL18 prevented unconventional T cell priming, resulting in MHC-Ia-targeted responses. UL18 is homologous to MHC-I but does not engage T cell receptors and, instead, binds with high affinity to inhibitory leukocyte immunoglobulin-like receptor-1 (LIR-1). UL18 lacking LIR-1 binding no longer interfered with MHC-E-restricted T cell stimulation by RhCMV-infected cells or the induction of unconventionally restricted T cells. Thus, LIR-1 binding needs to be deleted from UL18 of HCMV/HIV vaccines to allow for the induction of protective MHC-E-restricted T cells.

Published

2024

4. CD8 + T cell targeting of tumor antigens presented by HLA-E.

Author

Iyer RF, Verweij MC, Nair SS, Morrow D, Mansouri M, Chakravarty D, Beechwood T, Meyer C, Uebelhoer L, Lauron EJ, Selseth A, John N, Thin TH, Dzedzik S, Havenar-Daughton C, Axthelm MK, Douglas J, Korman A, Bhardwaj N, Tewari AK, Hansen S, Malouli D, Picker LJ, and Früh K

Subjects

Animals, Humans, Male, Acid Phosphatase, Antigen Presentation immunology, Cancer Vaccines immunology, Cell Line, Tumor, Cytomegalovirus immunology, Histocompatibility Antigens Class I immunology, Histocompatibility Antigens Class I metabolism, Macaca mulatta, Mesothelin, Antigens, Neoplasm immunology, CD8-Positive T-Lymphocytes immunology, HLA-E Antigens

Abstract

The nonpolymorphic major histocompatibility complex E (MHC-E) molecule is up-regulated on many cancer cells, thus contributing to immune evasion by engaging inhibitory NKG2A/CD94 receptors on NK cells and tumor-infiltrating T cells. To investigate whether MHC-E expression by cancer cells can be targeted for MHC-E-restricted T cell control, we immunized rhesus macaques (RM) with rhesus cytomegalovirus (RhCMV) vectors genetically programmed to elicit MHC-E-restricted CD8 + T cells and to express established tumor-associated antigens (TAAs) including prostatic acidic phosphatase (PAP), Wilms tumor-1 protein, or Mesothelin. T cell responses to all three tumor antigens were comparable to viral antigen-specific responses with respect to frequency, duration, phenotype, epitope density, and MHC restriction. Thus, CMV-vectored cancer vaccines can bypass central tolerance by eliciting T cells to noncanonical epitopes. We further demonstrate that PAP-specific, MHC-E-restricted CD8 + T cells from RhCMV/PAP-immunized RM respond to PAP-expressing HLA-E + prostate cancer cells, suggesting that the HLA-E/NKG2A immune checkpoint can be exploited for CD8 + T cell-based immunotherapies.

Published

2024

5. Late gene expression-deficient cytomegalovirus vectors elicit conventional T cells that do not protect against SIV.

Author

Hansen SG, Womack JL, Perez W, Schmidt KA, Marshall E, Iyer RF, Cleveland Rubeor H, Otero CE, Taher H, Vande Burgt NH, Barfield R, Randall KT, Morrow D, Hughes CM, Selseth AN, Gilbride RM, Ford JC, Caposio P, Tarantal AF, Chan C, Malouli D, Barry PA, Permar SR, Picker LJ, and Früh K

Subjects

Animals, Humans, Macaca mulatta, Gene Expression, Cytomegalovirus genetics, Simian Immunodeficiency Virus

Abstract

Rhesus cytomegalovirus-based (RhCMV-based) vaccine vectors induce immune responses that protect ~60% of rhesus macaques (RMs) from SIVmac239 challenge. This efficacy depends on induction of effector memory-based (EM-biased) CD8+ T cells recognizing SIV peptides presented by major histocompatibility complex-E (MHC-E) instead of MHC-Ia. The phenotype, durability, and efficacy of RhCMV/SIV-elicited cellular immune responses were maintained when vector spread was severely reduced by deleting the antihost intrinsic immunity factor phosphoprotein 71 (pp71). Here, we examined the impact of an even more stringent attenuation strategy on vector-induced immune protection against SIV. Fusion of the FK506-binding protein (FKBP) degradation domain to Rh108, the orthologue of the essential human CMV (HCMV) late gene transcription factor UL79, generated RhCMV/SIV vectors that conditionally replicate only when the FK506 analog Shield-1 is present. Despite lacking in vivo dissemination and reduced innate and B cell responses to vaccination, Rh108-deficient 68-1 RhCMV/SIV vectors elicited high-frequency, durable, EM-biased, SIV-specific T cell responses in RhCMV-seropositive RMs at doses of ≥ 1 × 106 PFU. Strikingly, elicited CD8+ T cells exclusively targeted MHC-Ia-restricted epitopes and failed to protect against SIVmac239 challenge. Thus, Rh108-dependent late gene expression is required for both induction of MHC-E-restricted T cells and protection against SIV.

Published

2023