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

Author

Hansen, Scott G, Womack, Jennie L, Perez, Wilma, Schmidt, Kimberli A, Marshall, Emily, Iyer, Ravi F, Cleveland-Rubeor, Hillary, Otero, Claire E, Taher, Husam, Burgt, Nathan H Vande, Barfield, Richard, Randall, Kurt T, Morrow, David, Hughes, Colette M, Selseth, Andrea N, Gilbride, Roxanne M, Ford, Julia C, Caposio, Patrizia, Tarantal, Alice, Chan, Cliburn, Malouli, Daniel, Barry, Peter A, Permar, Sallie R, Picker, Louis J, and Frueh, Klaus

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Vaccine Related (AIDS), Prevention, Immunization, Infectious Diseases, Genetics, Vaccine Related, HIV/AIDS, Sexually Transmitted Infections, Infection, Good Health and Well Being, Animals, Humans, Cytomegalovirus, Simian Immunodeficiency Virus, Macaca mulatta, Gene Expression, Simian immunodeficiency virus, AIDS vaccine, AIDS/HIV, T cells, Virology, Biomedical and clinical sciences, Health sciences
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

2. Reduced Cell Surface Levels of C-C Chemokine Receptor 5 and Immunosuppression in Long Coronavirus Disease 2019 Syndrome

Author

Gaylis, Norman B, Ritter, Angela, Kelly, Scott A, Pourhassan, Nader Z, Tiwary, Meenakshi, Sacha, Jonah B, Hansen, Scott G, Recknor, Christopher, and Yang, Otto O

Subjects
Clinical Research, Clinical Trials and Supportive Activities, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Good Health and Well Being, COVID-19, Chemokines, CC, Humans, Immunosuppression Therapy, Receptors, CCR5, CCR5, leronlimab, long COVID, immunosuppression, Biological Sciences, Medical and Health Sciences, Microbiology
Abstract

In an exploratory trial treating "long COVID" with the CCR5-binding antibody leronlimab, we observed significantly increased blood cell surface CCR5 in treated symptomatic responders but not in nonresponders or placebo-treated participants. These findings suggest an unexpected mechanism of abnormal immune downmodulation in some persons that is normalized by leronlimab. Clinical Trials Registration. NCT04678830.

Published
2022

3. Identification and Characterization of Antigen-Specific CD8+ T Cells Using Surface-Trapped TNF-α and Single-Cell Sequencing.

Author

Abdulhaqq, Shaheed, Ventura, Abigail B, Reed, Jason S, Bashirova, Arman A, Bateman, Katherine B, McDonald, Eric, Wu, Helen L, Greene, Justin M, Schell, John B, Morrow, David, Wisskirchen, Karin, Martin, Jeffrey N, Deeks, Steven G, Carrington, Mary, Protzer, Ulrike, Früh, Klaus, Hansen, Scott G, Picker, Louis J, Sacha, Jonah B, and Bimber, Benjamin N

Subjects
Biomedical and Clinical Sciences, Immunology, Infectious Diseases, HIV/AIDS, Sexually Transmitted Infections, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, Infection, Good Health and Well Being, Animals, CD8-Positive T-Lymphocytes, Epitopes, Epitopes, T-Lymphocyte, HIV Infections, Macaca mulatta, Receptors, Antigen, T-Cell, Tumor Necrosis Factor-alpha, Biochemistry and cell biology
Abstract

CD8+ T cells are key mediators of antiviral and antitumor immunity. The isolation and study of Ag-specific CD8+ T cells, as well as mapping of their MHC restriction, has practical importance to the study of disease and the development of therapeutics. Unfortunately, most experimental approaches are cumbersome, owing to the highly variable and donor-specific nature of MHC-bound peptide/TCR interactions. Here we present a novel system for rapid identification and characterization of Ag-specific CD8+ T cells, particularly well suited for samples with limited primary cells. Cells are stimulated ex vivo with Ag of interest, followed by live cell sorting based on surface-trapped TNF-α. We take advantage of major advances in single-cell sequencing to generate full-length sequence data from the paired TCR α- and β-chains from these Ag-specific cells. The paired TCR chains are cloned into retroviral vectors and used to transduce donor CD8+ T cells. These TCR transductants provide a virtually unlimited experimental reagent, which can be used for further characterization, such as minimal epitope mapping or identification of MHC restriction, without depleting primary cells. We validated this system using CMV-specific CD8+ T cells from rhesus macaques, characterizing an immunodominant Mamu-A1*002:01-restricted epitope. We further demonstrated the utility of this system by mapping a novel HLA-A*68:02-restricted HIV Gag epitope from an HIV-infected donor. Collectively, these data validate a new strategy to rapidly identify novel Ags and characterize Ag-specific CD8+ T cells, with applications ranging from the study of infectious disease to immunotherapeutics and precision medicine.

Published
2021

5. In vitro and in vivo characterization of a recombinant rhesus cytomegalovirus containing a complete genome

Author

Taher, Husam, Mahyari, Eisa, Kreklywich, Craig, Uebelhoer, Luke S, McArdle, Matthew R, Moström, Matilda J, Bhusari, Amruta, Nekorchuk, Michael, E, Xiaofei, Whitmer, Travis, Scheef, Elizabeth A, Sprehe, Lesli M, Roberts, Dawn L, Hughes, Colette M, Jackson, Kerianne A, Selseth, Andrea N, Ventura, Abigail B, Cleveland-Rubeor, Hillary C, Yue, Yujuan, Schmidt, Kimberli A, Shao, Jason, Edlefsen, Paul T, Smedley, Jeremy, Kowalik, Timothy F, Stanton, Richard J, Axthelm, Michael K, Estes, Jacob D, Hansen, Scott G, Kaur, Amitinder, Barry, Peter A, Bimber, Benjamin N, Picker, Louis J, Streblow, Daniel N, Früh, Klaus, and Malouli, Daniel

Subjects
Infectious Diseases, Biotechnology, Genetics, 2.2 Factors relating to the physical environment, Aetiology, Infection, Animals, Cell Line, Chromosomes, Artificial, Bacterial, Cytomegalovirus, Cytomegalovirus Infections, DNA, Recombinant, Disease Models, Animal, Female, Fibroblasts, Genome, Viral, Humans, Macaca mulatta, Male, Mutation, Open Reading Frames, Phylogeny, Species Specificity, Viremia, Microbiology, Immunology, Medical Microbiology, Virology
Abstract

Cytomegaloviruses (CMVs) are highly adapted to their host species resulting in strict species specificity. Hence, in vivo examination of all aspects of CMV biology employs animal models using host-specific CMVs. Infection of rhesus macaques (RM) with rhesus CMV (RhCMV) has been established as a representative model for infection of humans with HCMV due to the close evolutionary relationships of both host and virus. However, the only available RhCMV clone that permits genetic modifications is based on the 68-1 strain which has been passaged in fibroblasts for decades resulting in multiple genomic changes due to tissue culture adaptations. As a result, 68-1 displays reduced viremia in RhCMV-naïve animals and limited shedding compared to non-clonal, low passage isolates. To overcome this limitation, we used sequence information from primary RhCMV isolates to construct a full-length (FL) RhCMV by repairing all mutations affecting open reading frames (ORFs) in the 68-1 bacterial artificial chromosome (BAC). Inoculation of adult, immunocompetent, RhCMV-naïve RM with the reconstituted virus resulted in significant viremia in the blood similar to primary isolates of RhCMV and furthermore led to high viral genome copy numbers in many tissues at day 14 post infection. In contrast, viral dissemination was greatly reduced upon deletion of genes also lacking in 68-1. Transcriptome analysis of infected tissues further revealed that chemokine-like genes deleted in 68-1 are among the most highly expressed viral transcripts both in vitro and in vivo consistent with an important immunomodulatory function of the respective proteins. We conclude that FL-RhCMV displays in vitro and in vivo characteristics of a wildtype virus while being amenable to genetic modifications through BAC recombineering techniques.

Published
2020

7. Interferon‐Gamma test for the detection of Mycobacterium tuberculosis complex infection in Macaca mulatta and other non‐human primates

Author

Yee, JoAnn L, Prongay, Kamm, Miles, Brodie, Smedley, Jeremy, Hansen, Scott G, Axthelm, Michael K, Ardeshir, Amir, Van Rompay, Koen KA, Timmel, Gregory, and Roberts, Jeffrey A

Subjects
Veterinary Sciences, Agricultural, Veterinary and Food Sciences, Emerging Infectious Diseases, Biodefense, Prevention, HIV/AIDS, Rare Diseases, Tuberculosis, Vaccine Related, Infectious Diseases, Aetiology, 2.2 Factors relating to the physical environment, Infection, Good Health and Well Being, Animals, Enzyme-Linked Immunosorbent Assay, Interferon-gamma Release Tests, Macaca mulatta, Monkey Diseases, Mycobacterium tuberculosis, cell-mediated immune response, interferon-gamma release assay, purified protein derivative-tuberculin, Zoology, Virology, Veterinary sciences
Abstract

We have formatted an assay to detect Mycobacterium tuberculosis complex infections of non-human primates. Commercially available reagents were used to elicit a specific immune response that was measured by interferon-gamma release. Initial evaluation using blood samples from Rhesus macaques experimentally infected with M tuberculosis distinguished infected versus uninfected animals.

Published
2019

8. Acute Infection and Subsequent Subclinical Reactivation of Herpes Simplex Virus 2 after Vaginal Inoculation of Rhesus Macaques

Author

Lo, Ming, Zhu, Jia, Hansen, Scott G, Carroll, Timothy, Zuend, Christina Farr, Nöel-Romas, Laura, Ma, Zhong-Min, Fritts, Linda, Huang, Meei-Li, Sun, Sijie, Huang, Ying, Koelle, David M, Picker, Louis J, Burgener, Adam, Corey, Lawrence, and Miller, Christopher J

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, HIV/AIDS, Sexually Transmitted Infections, Prevention, Infectious Diseases, 2.1 Biological and endogenous factors, 2.2 Factors relating to the physical environment, Infection, Good Health and Well Being, Acantholysis, Animals, Disease Models, Animal, Female, Herpes Simplex, Herpesvirus 2, Human, Humans, Macaca mulatta, T-Lymphocytes, Vagina, Virus Latency, Virus Shedding, female reproductive tract, T-cell responses, cervix, herpes simplex virus, proteomics, subclinical infection, vaginal swabs, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology, Agricultural, veterinary and food sciences, Biological sciences, Biomedical and clinical sciences
Abstract

Herpes simplex virus 2 (HSV-2) is a common sexually transmitted infection with a highly variable clinical course. Many infections quickly become subclinical, with episodes of spontaneous virus reactivation. To study host-HSV-2 interactions, an animal model of subclinical HSV-2 infection is needed. In an effort to develop a relevant model, rhesus macaques (RM) were inoculated intravaginally with two or three HSV-2 strains (186, 333, and/or G) at a total dose of 1 × 107 PFU of HSV-2 per animal. Infectious HSV-2 and HSV-2 DNA were consistently shed in vaginal swabs for the first 7 to 14 days after each inoculation. Proteins associated with wound healing, innate immunity, and inflammation were significantly increased in cervical secretions immediately after HSV-2 inoculation. There was histologic evidence of acute herpesvirus pathology, including acantholysis in the squamous epithelium and ballooning degeneration of and intranuclear inclusion bodies in epithelial cells, with HSV antigen in mucosal epithelial cells and keratinocytes. Further, an intense inflammatory infiltrate was found in the cervix and vulva. Evidence of latent infection and reactivation was demonstrated by the detection of spontaneous HSV-2 shedding post-acute inoculation (102 to 103 DNA copies/swab) in 80% of RM. Further, HSV-2 DNA was detected in ganglia in most necropsied animals. HSV-2-specifc T-cell responses were detected in all animals, although antibodies to HSV-2 were detected in only 30% of the animals. Thus, HSV-2 infection of RM recapitulates many of the key features of subclinical HSV-2 infection in women but seems to be more limited, as virus shedding was undetectable more than 40 days after the last virus inoculation.IMPORTANCE Herpes simplex virus 2 (HSV-2) infects nearly 500 million persons globally, with an estimated 21 million incident cases each year, making it one of the most common sexually transmitted infections (STIs). HSV-2 is associated with increased human immunodeficiency virus type 1 (HIV-1) acquisition, and this risk does not decline with the use of antiherpes drugs. As initial acquisition of both HIV and HSV-2 infections is subclinical, study of the initial molecular interactions of the two agents requires an animal model. We found that HSV-2 can infect RM after vaginal inoculation, establish latency in the nervous system, and spontaneously reactivate; these features mimic some of the key features of HSV-2 infection in women. RM may provide an animal model to develop strategies to prevent HSV-2 acquisition and reactivation.

Published
2019

9. Functional genomic analysis of the 68-1 RhCMV-Mycobacteria tuberculosis vaccine reveals an IL-15 response signature that is conserved with vector attenuation.

Author

Cheng-Jung Sung, Whitmore, Leanne S., Smith, Elise, Chang, Jean, Tisoncik-Go, Jennifer, Barber-Axthelm, Aaron, Selseth, Andrea, Feltham, Shana, Ojha, Sohita, Hansen, Scott G., Picker, Louis J., and Gale Jr., Michael

Subjects
SIMIAN immunodeficiency virus, MYCOBACTERIUM tuberculosis, TUBERCULOSIS vaccines, RHESUS monkeys, IMMUNOLOGIC memory
Abstract

Tuberculosis (TB), caused by Mycobacterium tuberculosis (Mtb) is a deadly infectious disease having a major impact on global health. Using the CMV vector for development of novel vaccines is a promising new strategy that elicits strong and durable, high frequency memory T cell responses against heterologous immunogens. We conducted functional transcriptomic analysis of whole blood samples collected from cohorts of rhesus (Rh) macaques that were administered RhCMV/TB vector using a prime-boost strategy. Two modified CMV vectors were used in this study, including 68-1 RhCMV/TB-6Ag (encoding 6 Mtb protein immunogens, including Ag85A, ESAT-6, Rv3407, Rv2626, Rpf A, and Rpf D) and its attenuated variant, 68-1 RhCMV/Dpp71-TB-6Ag (a cell-to-cell spread-deficient vaccine vector lacking the Rh110 gene encoding the pp71 tegument protein). Bulk mRNA sequencing, differential gene expression, and functional enrichment analyses showed that these RhCMV/TB vaccines induce the innate and adaptive immune responses with specific transcriptomic signatures, including the IL-15-induced protective gene signature previously defined to be linked with protection against simian immunodeficiency virus (SIV) by the 68-1 RhCMV/SIV vaccine. While both vectors exhibited a transcriptomic response of the IL-15 protective signature in whole blood, we show that lack of pp71 does not maintain induction of the protective signature for the full duration of the study compared to the parental non-attenuated vector. Our observations indicate that RhCMV vector vaccines induce a transcriptomic response in whole blood that include a conserved IL-15 signature of which vector-encoded pp71 is an important component of response durability that upon future Mtb challenge may define specific vaccine protection outcomes against Mtb infection. [ABSTRACT FROM AUTHOR]

Published
2024
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10. 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
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11. Viral escape mutations do not account for non-protection from SIVmac239 challenge in RhCMV/SIV vaccinated rhesus macaques.

Author

Bimber, Benjamin N., Sunshine, Justine, McElfresh, G. W., Reed, Jason S., Pathak, Reese, Bateman, Katherine B., Hughes, Colette M., Gilbride, Roxanne M., Ford, Julia C., Morrow, David, Lifson, Jeffrey D., Sacha, Jonah B., Hansen, Scott G., and Picker, Louis J.

Subjects
VIRAL mutation, SIMIAN immunodeficiency virus, RHESUS monkeys, VACCINATION status, T cells
Abstract

Simian immunodeficiency virus (SIV) vaccines based upon 68-1 Rhesus Cytomegalovirus (RhCMV) vectors show remarkable protection against pathogenic SIVmac239 challenge. Across multiple independent rhesus macaque (RM) challenge studies, nearly 60% of vaccinated RM show early, complete arrest of SIVmac239 replication after effective challenge, whereas the remainder show progressive infection similar to controls. Here, we performed viral sequencing to determine whether the failure to control viral replication in non-protected RMs is associated with the acquisition of viral escape mutations. While low level viral mutations accumulated in all animals by 28 days-post-challenge, which is after the establishment of viral control in protected animals, the dominant circulating virus in virtually all unprotected RMs was nearly identical to the challenge stock, and there was no difference in mutation patterns between this cohort and unvaccinated controls. These data definitively demonstrate that viral mutation does not explain lack of viral control in RMs not protected by RhCMV/SIV vaccination. We further demonstrate that during chronic infection RhCMV/SIV vaccinated RMs do not acquire escape mutation in epitopes targeted by RhCMV/SIV, but instead display mutation in canonical MHC-Ia epitopes similar to unvaccinated RMs. This suggests that after the initial failure of viral control, unconventional T cell responses induced by 68-1 RhCMV/SIV vaccination do not exert strong selective pressure on systemically replicating SIV. [ABSTRACT FROM AUTHOR]

Published
2024
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13. Rhesus Cytomegalovirus-encoded Fcγ-binding glycoproteins facilitate viral evasion from IgG-mediated humoral immunity

Author

Otero, Claire E., primary, Petkova, Sophia, additional, Ebermann, Martin, additional, Taher, Husam, additional, John, Nessy, additional, Hoffmann, Katja, additional, Davalos, Angel, additional, Mostrom, Matilda J, additional, Gilbride, Roxanne M, additional, Papen, Courtney, additional, Barber-Axthelm, Aaron, additional, Scheef, Elizabeth A., additional, Barfield, Richard, additional, Sprehe, Lesli M., additional, Kendall, Savannah, additional, Manuel, Tabitha D, additional, Vande Burgt, Nathan, additional, Chan, Cliburn, additional, Streblow, Daniel N., additional, Hansen, Scott G., additional, Denton, Michael, additional, Streblow, Zachary, additional, Kaur, Amitinder, additional, Permar, Sallie R, additional, Frueh, Klaus, additional, Hengel, Hartmut, additional, Malouli, Daniel, additional, and Kolb, Philipp, additional

Published
2024
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14. TIGIT Marks Exhausted T Cells, Correlates with Disease Progression, and Serves as a Target for Immune Restoration in HIV and SIV Infection.

Author

Chew, Glen M, Fujita, Tsuyoshi, Webb, Gabriela M, Burwitz, Benjamin J, Wu, Helen L, Reed, Jason S, Hammond, Katherine B, Clayton, Kiera L, Ishii, Naoto, Abdel-Mohsen, Mohamed, Liegler, Teri, Mitchell, Brooks I, Hecht, Frederick M, Ostrowski, Mario, Shikuma, Cecilia M, Hansen, Scott G, Maurer, Mark, Korman, Alan J, Deeks, Steven G, Sacha, Jonah B, and Ndhlovu, Lishomwa C

Subjects
CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, Animals, Macaca mulatta, Humans, HIV Infections, Simian Acquired Immunodeficiency Syndrome, Disease Progression, Receptors, Immunologic, DNA, Viral, RNA, Viral, Flow Cytometry, Cell Separation, Lymphocyte Activation, B7-H1 Antigen, Receptors, Immunologic, DNA, Viral, RNA, Virology, Microbiology, Immunology, Medical Microbiology
Abstract

HIV infection induces phenotypic and functional changes to CD8+ T cells defined by the coordinated upregulation of a series of negative checkpoint receptors that eventually result in T cell exhaustion and failure to control viral replication. We report that effector CD8+ T cells during HIV infection in blood and SIV infection in lymphoid tissue exhibit higher levels of the negative checkpoint receptor TIGIT. Increased frequencies of TIGIT+ and TIGIT+ PD-1+ CD8+ T cells correlated with parameters of HIV and SIV disease progression. TIGIT remained elevated despite viral suppression in those with either pharmacological antiretroviral control or immunologically in elite controllers. HIV and SIV-specific CD8+ T cells were dysfunctional and expressed high levels of TIGIT and PD-1. Ex-vivo single or combinational antibody blockade of TIGIT and/or PD-L1 restored viral-specific CD8+ T cell effector responses. The frequency of TIGIT+ CD4+ T cells correlated with the CD4+ T cell total HIV DNA. These findings identify TIGIT as a novel marker of dysfunctional HIV-specific T cells and suggest TIGIT along with other checkpoint receptors may be novel curative HIV targets to reverse T cell exhaustion.

Published
2016

15. Antibody-based CCR5 blockade protects Macaques from mucosal SHIV transmission

Author

Chang, Xiao L., Webb, Gabriela M., Wu, Helen L., Greene, Justin M., Abdulhaqq, Shaheed, Bateman, Katherine B., Reed, Jason S., Pessoa, Cleiton, Weber, Whitney C., Maier, Nicholas, Chew, Glen M., Gilbride, Roxanne M., Gao, Lina, Agnor, Rebecca, Giobbi, Travis, Torgerson, Jeffrey, Siess, Don, Burnett, Nicole, Fischer, Miranda, Shiel, Oriene, Moats, Cassandra, Patterson, Bruce, Dhody, Kush, Kelly, Scott, Pourhassan, Nader, Magnani, Diogo M., Smedley, Jeremy, Bimber, Benjamin N., Haigwood, Nancy L., Hansen, Scott G., Brown, Timothy R., Ndhlovu, Lishomwa C., and Sacha, Jonah B.

Published
2021
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16. Expansion of Dysfunctional Tim-3–Expressing Effector Memory CD8+ T Cells during Simian Immunodeficiency Virus Infection in Rhesus Macaques

Author

Fujita, Tsuyoshi, Burwitz, Benjamin J, Chew, Glen M, Reed, Jason S, Pathak, Reesab, Seger, Elizabeth, Clayton, Kiera L, Rini, James M, Ostrowski, Mario A, Ishii, Naoto, Kuroda, Marcelo J, Hansen, Scott G, Sacha, Jonah B, and Ndhlovu, Lishomwa C

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, HIV/AIDS, Sexually Transmitted Infections, Immunotherapy, Aetiology, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Acquired Immunodeficiency Syndrome, Amino Acid Sequence, Animals, CD8-Positive T-Lymphocytes, Cell Proliferation, Cells, Cultured, Cytotoxicity, Immunologic, Disease Models, Animal, Gene Expression Regulation, Hepatitis A Virus Cellular Receptor 2, Humans, Immunologic Memory, Macaca mulatta, Membrane Proteins, Molecular Sequence Data, Molecular Targeted Therapy, Programmed Cell Death 1 Receptor, Simian Acquired Immunodeficiency Syndrome, Simian Immunodeficiency Virus, Viral Load, Virus Replication, Simian immunodeficiency virus, Biochemistry and cell biology
Abstract

The T cell Ig- and mucin domain-containing molecule-3 (Tim-3) negative immune checkpoint receptor demarcates functionally exhausted CD8(+) T cells arising from chronic stimulation in viral infections like HIV. Tim-3 blockade leads to improved antiviral CD8(+) T cell responses in vitro and, therefore, represents a novel intervention strategy to restore T cell function in vivo and protect from disease progression. However, the Tim-3 pathway in the physiologically relevant rhesus macaque SIV model of AIDS remains uncharacterized. We report that Tim-3(+)CD8(+) T cell frequencies are significantly increased in lymph nodes, but not in peripheral blood, in SIV-infected animals. Tim-3(+)PD-1(+)CD8(+) T cells are similarly increased during SIV infection and positively correlate with SIV plasma viremia. Tim-3 expression was found primarily on effector memory CD8(+) T cells in all tissues examined. Tim-3(+)CD8(+) T cells have lower Ki-67 content and minimal cytokine responses to SIV compared with Tim-3(-)CD8(+) T cells. During acute-phase SIV replication, Tim-3 expression peaked on SIV-specific CD8(+) T cells by 2 wk postinfection and then rapidly diminished, irrespective of mutational escape of cognate Ag, suggesting non-TCR-driven mechanisms for Tim-3 expression. Thus, rhesus Tim-3 in SIV infection partially mimics human Tim-3 in HIV infection and may serve as a novel model for targeted studies focused on rejuvenating HIV-specific CD8(+) T cell responses.

Published
2014

17. The pentameric complex is not required for vertical transmission of cytomegalovirus in seronegative pregnant rhesus macaques

Author

Wang, Hsuan-Yuan, primary, Taher, Husam, additional, Kreklywich, Craig N., additional, Schmidt, Kimberli A., additional, Scheef, Elizabeth A., additional, Barfield, Richard, additional, Otero, Claire E., additional, Valencia, Sarah M., additional, Crooks, Chelsea M., additional, Mirza, Anne, additional, Woods, Kelsey, additional, Burgt, Nathan Vande, additional, Kowalik, Timothy F., additional, Barry, Peter A., additional, Hansen, Scott G., additional, Tarantal, Alice F., additional, Chan, Cliburn, additional, Streblow, Daniel N., additional, Picker, Louis J., additional, Kaur, Amitinder, additional, Früh, Klaus, additional, Permar, Sallie R., additional, and Malouli, Daniel, additional

Published
2023
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18. Characterization of a live-attenuated HCMV-based vaccine platform

Author

Caposio, Patrizia, van den Worm, Sjoerd, Crawford, Lindsey, Perez, Wilma, Kreklywich, Craig, Gilbride, Roxanne M., Hughes, Colette M., Ventura, Abigail B., Ratts, Robert, Marshall, Emily E., Malouli, Daniel, Axthelm, Michael K., Streblow, Daniel, Nelson, Jay A., Picker, Louis J., Hansen, Scott G., and Früh, Klaus

Published
2019
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19. The pentameric complex is not required for vertical transmission of cytomegalovirus in seronegative pregnant rhesus macaques

Author

Wang, Hsuan-Yuan, Taher, Husam, Kreklywich, Craig N., Schmidt, Kimberli A., Scheef, Elizabeth A., Barfield, Richard, Otero, Claire E., Valencia, Sarah M., Crooks, Chelsea M., Mirza, Anne, Woods, Kelsey, Burgt, Nathan Vande, Kowalik, Timothy F., Barry, Peter A., Hansen, Scott G., Tarantal, Alice F., Chan, Cliburn, Streblow, Daniel N., Picker, Louis J., Kaur, Amitinder, Früh, Klaus, Permar, Sallie R., and Malouli, Daniel

Subjects
Article
Abstract

Congenital cytomegalovirus (cCMV) infection is the leading infectious cause of neonatal neurological impairment but essential virological determinants of transplacental CMV transmission remain unclear. The pentameric complex (PC), composed of five subunits, glycoproteins H (gH), gL, UL128, UL130, and UL131A, is essential for efficient entry into non-fibroblast cells in vitro . Based on this role in cell tropism, the PC is considered a possible target for CMV vaccines and immunotherapies to prevent cCMV. To determine the role of the PC in transplacental CMV transmission in a non-human primate model of cCMV, we constructed a PC-deficient rhesus CMV (RhCMV) by deleting the homologues of the HCMV PC subunits UL128 and UL130 and compared congenital transmission to PC-intact RhCMV in CD4+ T cell-depleted or immunocompetent RhCMV-seronegative, pregnant rhesus macaques (RM). Surprisingly, we found that the transplacental transmission rate was similar for PC-intact and PC-deleted RhCMV based on viral genomic DNA detection in amniotic fluid. Moreover, PC-deleted and PC-intact RhCMV acute infection led to similar peak maternal plasma viremia. However, there was less viral shedding in maternal urine and saliva and less viral dissemination in fetal tissues in the PC-deleted group. As expected, dams inoculated with PC-deleted RhCMV demonstrated lower plasma IgG binding to PC-intact RhCMV virions and soluble PC, as well as reduced neutralization of PC-dependent entry of the PC-intact RhCMV isolate UCD52 into epithelial cells. In contrast, binding to gH expressed on the cell surface and neutralization of entry into fibroblasts by the PC-intact RhCMV was higher for dams infected with PC-deleted RhCMV compared to those infected with PC-intact RhCMV. Our data demonstrates that the PC is dispensable for transplacental CMV infection in our non-human primate model. ONE SENTENCE SUMMARY: Congenital CMV transmission frequency in seronegative rhesus macaques is not affected by the deletion of the viral pentameric complex.

Published
2023

20. Prevention of tuberculosis in rhesus macaques by a cytomegalovirus-based vaccine

Author

Hansen, Scott G, Zak, Daniel E, Xu, Guangwu, Ford, Julia C, Marshall, Emily E, Malouli, Daniel, Gilbride, Roxanne M, Hughes, Colette M, Ventura, Abigail B, Ainslie, Emily, Randall, Kurt T, Selseth, Andrea N, Rundstrom, Parker, Herlache, Lauren, Lewis, Matthew S, Park, Haesun, Planer, Shannon L, Turner, John M, Fischer, Miranda, Armstrong, Christina, Zweig, Robert C, Valvo, Joseph, Braun, Jackie M, Shankar, Smitha, Lu, Lenette, Sylwester, Andrew W, Legasse, Alfred W, Messerle, Martin, Jarvis, Michael A, Amon, Lynn M, Aderem, Alan, Alter, Galit, Laddy, Dominick J, Stone, Michele, Bonavia, Aurelio, Evans, Thomas G, Axthelm, Michael K, Früh, Klaus, Edlefsen, Paul T, and Picker, Louis J

Subjects
Tuberculosis vaccines -- Comparative analysis -- Physiological aspects -- Genetic aspects -- Research, Tuberculosis -- Prevention -- Comparative analysis -- Genetic aspects -- Research, T cells -- Comparative analysis -- Physiological aspects -- Genetic aspects -- Research, Biological sciences, Health
Abstract

Despite widespread use of the bacille Calmette-Guérin (BCG) vaccine, tuberculosis (TB) remains a leading cause of global mortality from a single infectious agent (Mycobacterium tuberculosis or Mtb). Here, over two independent Mtb challenge studies, we demonstrate that subcutaneous vaccination of rhesus macaques (RMs) with rhesus cytomegalovirus vectors encoding Mtb antigen inserts (hereafter referred to as RhCMV/TB)--which elicit and maintain highly effector-differentiated, circulating and tissue-resident Mtb-specific CD4[sup.+] and CD8[sup.+] memory T cell responses--can reduce the overall (pulmonary and extrapulmonary) extent of Mtb infection and disease by 68%, as compared to that in unvaccinated controls, after intrabronchial challenge with the Erdman strain of Mtb at [similar]1 year after the first vaccination. Fourteen of 34 RhCMV/TB-vaccinated RMs (41%) across both studies showed no TB disease by computed tomography scans or at necropsy after challenge (as compared to 0 of 17 unvaccinated controls), and ten of these RMs were Mtb-culture-negative for all tissues, an exceptional long-term vaccine effect in the RM challenge model with the Erdman strain of Mtb. These results suggest that complete vaccine-mediated immune control of highly pathogenic Mtb is possible if immune effector responses can intercept Mtb infection at its earliest stages., Author(s): Scott G Hansen [1]; Daniel E Zak [2]; Guangwu Xu [1]; Julia C Ford [1]; Emily E Marshall [1]; Daniel Malouli [1]; Roxanne M Gilbride [1]; Colette M Hughes [...]

Published
2018
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21. Correction: Mitigation of endemic GI-tract pathogen-mediated inflammation through development of multimodal treatment regimen and its impact on SIV acquisition in rhesus macaques

Author

Bochart, Rachele M., primary, Busman-Sahay, Kathleen, additional, Bondoc, Stephen, additional, Morrow, David W., additional, Ortiz, Alexandra M., additional, Fennessey, Christine M., additional, Fischer, Miranda B., additional, Shiel, Oriene, additional, Swanson, Tonya, additional, Shriver-Munsch, Christine M., additional, Crank, Hugh B., additional, Armantrout, Kimberly M., additional, Barber-Axthelm, Aaron M., additional, Langner, Charlotte, additional, Moats, Cassandra R., additional, Labriola, Caralyn S., additional, MacAllister, Rhonda, additional, Axthelm, Michael K., additional, Brenchley, Jason M., additional, Keele, Brandon F., additional, Estes, Jacob D., additional, Hansen, Scott G., additional, and Smedley, Jeremy V., additional

Published
2023
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22. Broadly targeted CD8⁺ T cell responses restricted by major histocompatibility complex E

Author

Hansen, Scott G., Wu, Helen L., Burwitz, Benjamin J., Hughes, Colette M., Hammond, Katherine B., Ventura, Abigail B., Reed, Jason S., Gilbride, Roxanne M., Ainslie, Emily, Morrow, David W., Ford, Julia C., Selseth, Andrea N., Pathak, Reesab, Malouli, Daniel, Legasse, Alfred W., Axthelm, Michael K., Nelson, Jay A., Gillespie, Geraldine M., Walters, Lucy C., Brackenridge, Simon, Sharpe, Hannah R., López, César A., Früh, Klaus, Korber, Bette T., McMichael, Andrew J., Gnanakaran, S., Sacha, Jonah B., and Picker, Louis J.

Published
2016

23. T cells fail to limit SIV reactivation following ART withdrawal until after viral amplification

Author

Okoye, Afam A., Duell, Derick D., Fukazawa, Yoshinori, Varco-Merth, Benjamin, Marenco, Alejandra, Behrens, Hannah, Chaunzwa, Morgan, Selseth, Andrea N., Gilbride, Roxanne M., Shao, Jason, Edlefsen, Paul T., Geleziunas, Romas, Pinkevych, Mykola, Davenport, Miles P., Busman-Sahay, Kathleen, Nekorchuk, Michael, Park, Haesun, Smedley, Jeremy, Axthelm, Michael K., Estes, Jacob D., Hansen, Scott G., Keele, Brandon F., Lifson, Jeffery D., and Picker, Louis J.

Subjects
CD8 lymphocytes -- Health aspects, Antiviral agents -- Patient outcomes, Health care industry
Abstract

To define the contribution of [CD8.sup.+] T cell responses to control of SIV reactivation during and following antiretroviral therapy (ART), we determined the effect of long-term [CD8.sup.+] T cell depletion using a rhesusized anti-CD8|5 monoclonal antibody on barcoded SIVmac239 dynamics on stable ART and after ART cessation in rhesus macaques (RMs). Among the RMs with full [CD8.sup.+] T cell depletion in both blood and tissue, there were no significant differences in the frequency of viral blips in plasma, the number of SIV [RNA.sup.+] cells and the average number of RNA copies/infected cell in tissue, and levels of cell-associated SIV RNA and DNA in blood and tissue relative to control-treated RMs during ART. Upon ART cessation, both [CD8.sup.+] T cell-depleted and control RMs rebounded in fewer than 12 days, with no difference in the time to viral rebound or in either the number or growth rate of rebounding SIVmac239M barcode clonotypes. However, effectively [CD8.sup.+] T cell-depleted RMs showed a stable, approximately 2-log increase in post-ART plasma viremia relative to controls. These results indicate that while potent antiviral [CD8.sup.+] T cell responses can develop during ART-suppressed SIV infection, these responses effectively intercept post-ART SIV rebound only after systemic viral replication, too late to limit reactivation frequency or the early spread of reactivating SIV reservoirs., Introduction [CD8.sup.+] T cells are crucial components of the adaptive immune response against HIV and SIV, and most examples of stringent, long-term, spontaneous and vaccine-associated immune control of these infections [...]

Published
2021
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24. Cytomegalovirus-vaccine-induced unconventional T cell priming and control of SIV replication is conserved between primate species

Author

Malouli, Daniel, primary, Gilbride, Roxanne M., additional, Wu, Helen L., additional, Hwang, Joseph M., additional, Maier, Nicholas, additional, Hughes, Colette M., additional, Newhouse, Daniel, additional, Morrow, David, additional, Ventura, Abigail B., additional, Law, Lynn, additional, Tisoncik-Go, Jennifer, additional, Whitmore, Leanne, additional, Smith, Elise, additional, Golez, Inah, additional, Chang, Jean, additional, Reed, Jason S., additional, Waytashek, Courtney, additional, Weber, Whitney, additional, Taher, Husam, additional, Uebelhoer, Luke S., additional, Womack, Jennie L., additional, McArdle, Matthew R., additional, Gao, Junwei, additional, Papen, Courtney R., additional, Lifson, Jeffrey D., additional, Burwitz, Benjamin J., additional, Axthelm, Michael K., additional, Smedley, Jeremy, additional, Früh, Klaus, additional, Gale, Michael, additional, Picker, Louis J., additional, Hansen, Scott G., additional, and Sacha, Jonah B., additional

Published
2022
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25. Author Correction: Pathogen-derived HLA-E bound epitopes reveal broad primary anchor pocket tolerability and conformationally malleable peptide binding

Author

Walters, Lucy C., Harlos, Karl, Brackenridge, Simon, Rozbesky, Daniel, Barrett, Jordan R., Jain, Vitul, Walter, Thomas S., O’Callaghan, Chris A., Borrow, Persephone, Toebes, Mireille, Hansen, Scott G., Sacha, Jonah B., Abdulhaqq, Shaheed, Greene, Justin M., Früh, Klaus, Marshall, Emily, Picker, Louis J., Jones, E. Yvonne, McMichael, Andrew J., and Gillespie, Geraldine M.

Published
2018
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26. Pathogen-derived HLA-E bound epitopes reveal broad primary anchor pocket tolerability and conformationally malleable peptide binding

Author

Walters, Lucy C., Harlos, Karl, Brackenridge, Simon, Rozbesky, Daniel, Barrett, Jordan R., Jain, Vitul, Walter, Thomas S., O’Callaghan, Chris A., Borrow, Persephone, Toebes, Mireille, Hansen, Scott G., Sacha, Jonah B, Abdulhaqq, Shaheed, Greene, Justin M., Früh, Klaus, Marshall, Emily, Picker, Louis J., Jones, E. Yvonne, McMichael, Andrew J., and Gillespie, Geraldine M.

Published
2018
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27. Reply to Viel

Author

Recknor, Christopher, primary, Hansen, Scott G, additional, Gaylis, Norman B., additional, Tiwary, Meenakshi, additional, Sacha, Jonah B., additional, and Yang, Otto O, additional

Published
2022
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28. Myeloid cell tropism enables MHC-E–restricted CD8 + T cell priming and vaccine efficacy by the RhCMV/SIV vaccine

Author

Hansen, Scott G., primary, Hancock, Meaghan H., additional, Malouli, Daniel, additional, Marshall, Emily E., additional, Hughes, Colette M., additional, Randall, Kurt T., additional, Morrow, David, additional, Ford, Julia C., additional, Gilbride, Roxanne M., additional, Selseth, Andrea N., additional, Trethewy, Renee Espinosa, additional, Bishop, Lindsey M., additional, Oswald, Kelli, additional, Shoemaker, Rebecca, additional, Berkemeier, Brian, additional, Bosche, William J., additional, Hull, Michael, additional, Silipino, Lorna, additional, Nekorchuk, Michael, additional, Busman-Sahay, Kathleen, additional, Estes, Jacob D., additional, Axthelm, Michael K., additional, Smedley, Jeremy, additional, Shao, Danica, additional, Edlefsen, Paul T., additional, Lifson, Jeffrey D., additional, Früh, Klaus, additional, Nelson, Jay A., additional, and Picker, Louis J., additional

Published
2022
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29. Cytomegalovirus Vectors Violate CD8⁺ T Cell Epitope Recognition Paradigms

Author

Hansen, Scott G., Sacha, Jonah B., Hughes, Colette M., Ford, Julia C., Burwitz, Benjamin J., Scholz, Isabel, Gilbride, Roxanne M., Lewis, Matthew S., Gilliam, Awbrey N., Ventura, Abigail B., Malouli, Daniel, Xu, Guangwu, Richards, Rebecca, Whizin, Nathan, Reed, Jason S., Hammond, Katherine B., Fischer, Miranda, Turner, John M., Legasse, Alfred W., Axthelm, Michael K., Edlefsen, Paul T., Nelson, Jay A., Lifson, Jeffrey D., Früh, Klaus, and Picker, Louis J.

Published
2013
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30. T cell programming by the cytomegalovirus MHC class I homologue UL18

Author

Taher, Husam, primary, Malouli, Daniel, additional, Hansen, Scott G., additional, Mansouri, Mandana, additional, Iyer, Ravi, additional, Papen, Courtney, additional, Schell, John B., additional, Cleveland-Rubeor, Hillary, additional, McArdle, Matthew R., additional, Hughes, Colette M., additional, Randall, Kurt T., additional, McNett, Alisha, additional, Picker, Louis J., additional, and Früh, Klaus, additional

Published
2022
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31. Harnessing the unique immune biology of cytomegalovirus for cancer immunotherapy

Author

Iyer, L. Ravi F, primary, Verweij, Marieke C, additional, Nair, Sujit, additional, Morrow, David, additional, Mansouri, Mandana, additional, Beechwood, Teresa, additional, Meyer, Christine, additional, Chakravarty, Dimple, additional, Uebelhoer, Luke, additional, Ventura, Abigail, additional, Lauron, Elvin J, additional, Selseth, Andrea, additional, Axthelm, Michael, additional, Lind, Evan F, additional, Saultz, Jennifer, additional, Douglas, Janet, additional, Korman, Alan, additional, Bhardwaj, Nina, additional, Tewari, Ashutosh K, additional, Hansen, Scott G., additional, Malouli, Daniel, additional, Picker, Louis J, additional, and Fruh, Klaus, additional

Published
2022
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33. Suppression of human and simian immunodeficiency virus replication with the CCR5-specific antibody Leronlimab in two species

Author

Chang, Xiao L., primary, Reed, Jason S., additional, Webb, Gabriela M., additional, Wu, Helen L., additional, Le, Jimmy, additional, Bateman, Katherine B., additional, Greene, Justin M., additional, Pessoa, Cleiton, additional, Waytashek, Courtney, additional, Weber, Whitney C., additional, Hwang, Joseph, additional, Fischer, Miranda, additional, Moats, Cassandra, additional, Shiel, Oriene, additional, Bochart, Rachele M., additional, Crank, Hugh, additional, Siess, Don, additional, Giobbi, Travis, additional, Torgerson, Jeffrey, additional, Agnor, Rebecca, additional, Gao, Lina, additional, Dhody, Kush, additional, Lalezari, Jacob P., additional, Bandar, Ivo Sah, additional, Carnate, Alnor M., additional, Pang, Alina S., additional, Corley, Michael J., additional, Kelly, Scott, additional, Pourhassan, Nader, additional, Smedley, Jeremy, additional, Bimber, Benjamin N., additional, Hansen, Scott G., additional, Ndhlovu, Lishomwa C., additional, and Sacha, Jonah B., additional

Published
2022
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35. Cytomegalovirus pp65 limits dissemination but is dispensable for persistence

Author

Malouli, Daniel, Hansen, Scott G., Nakayasu, Ernesto S., Marshall, Emily E., Hughes, Colette M., Ventura, Abigail B., Gilbride, Roxanne M., Lewis, Matthew S., Xu, Guangwu, Kreklywich, Craig, Whizin, Nathan, Fischer, Miranda, Legasse, Alfred W., Viswanathan, Kasinath, Siess, Don, Camp, II, David G., Axthelm, Michael K., Kahl, Christoph, DeFilippis, Victor R., Smith, Richard D., Streblow, Daniel N., Picker, Louis J., and Fruh, Klaus

Subjects
Medical research, Medicine, Experimental, Vaccination -- Genetic aspects, Immune response -- Research, Viral proteins -- Properties, Health care industry
Abstract

The most abundantly produced virion protein in human cytomegalovirus (HCMV) is the immunodominant phosphoprotein 65 (pp65), which is frequently included in CMV vaccines. Although it is nonessential for in vitro CMV growth, pp65 displays immunomodulatory functions that support a potential role in primary and/or persistent infection. To determine the contribution of pp65 to CMV infection and immunity, we generated a rhesus CMV lacking both pp65 orthologs (RhCMVΔpp65ab). While deletion of pp65ab slightly reduced growth in vitro and increased defective particle formation, the protein composition of secreted virions was largely unchanged. Interestingly, pp65 was not required for primary and persistent infection in animals. Immune responses induced by RhCMVΔpp65ab did not prevent reinfection with rhesus CMV; however, reinfection with RhCMVΔUS2-11, which lacks viral-encoded MHC-I antigen presentation inhibitors, was prevented. Unexpectedly, induction of pp65b-specific T cells alone did not protect against RhCMVΔUS2-11 challenge, suggesting that T cells targeting multiple CMV antigens are required for protection. However, pp65-specific immunity was crucial for controlling viral dissemination during primary infection, as indicated by the marked increase of RhCMVΔpp65ab genome copies in CMV-naive, but not CMV-immune, animals. Our data provide rationale for inclusion of pp65 into CMV vaccines but also demonstrate that pp65-induced T cell responses alone do not recapitulate the protective effect of natural infection., Introduction Human cytomegalovirus (HCMV) persistently infects most of humanity (1). While the vast majority of these infections are asymptomatic and not associated with any pathologic consequence, HCMV can cause serious [...]

Published
2014
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36. IMMUNOLOGY: Broadly targeted CD8+ T cell responses restricted by major histocompatibility complex E

Author

Hansen, Scott G., Wu, Helen L., Burwitz, Benjamin J., Hughes, Colette M., Hammond, Katherine B., Ventura, Abigail B., Reed, Jason S., Gilbride, Roxanne M., Ainslie, Emily, Morrow, David W., Ford, Julia C., Selseth, Andrea N., Pathak, Reesab, Malouli, Daniel, Legasse, Alfred W., Axthelm, Michael K., Nelson, Jay A., Gillespie, Geraldine M., Walters, Lucy C., Brackenridge, Simon, Sharpe, Hannah R., López, César A., Früh, Klaus, Korber, Bette T., McMichael, Andrew J., Gnanakaran, S., Sacha, Jonah B., and Picker, Louis J.

Published
2016
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37. CCR5 Receptor Occupancy Analysis Reveals Increased Peripheral Blood CCR5+CD4+ T Cells Following Treatment With the Anti-CCR5 Antibody Leronlimab

Author

Chang, Xiao L., primary, Wu, Helen L., additional, Webb, Gabriela M., additional, Tiwary, Meenakshi, additional, Hughes, Colette, additional, Reed, Jason S., additional, Hwang, Joseph, additional, Waytashek, Courtney, additional, Boyle, Carla, additional, Pessoa, Cleiton, additional, Sylwester, Andrew W., additional, Morrow, David, additional, Belica, Karina, additional, Fischer, Miranda, additional, Kelly, Scott, additional, Pourhassan, Nader, additional, Bochart, Rachele M., additional, Smedley, Jeremy, additional, Recknor, Christopher P., additional, Hansen, Scott G., additional, and Sacha, Jonah B., additional

Published
2021
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40. Immune clearance of highly pathogenic SIV infection

Author

Hansen, Scott G., Jr, Michael Piatak, Ventura, Abigail B., Hughes, Colette M., Gilbride, Roxanne M., Ford, Julia C., Oswald, Kelli, Shoemaker, Rebecca, Li, Yuan, Lewis, Matthew S., Gilliam, Awbrey N., Xi, Guangwu, Nathan, Whizin, Burwitz, Benjamin J., Planer, Shannon L., Turner, John M., Legasse, Alfred W., Axthelm, Michael K., Nelson, Jay A., Fruh, Klaus, Sacha, Jonah B., Estes, Jacob D., Keele, Brandon F., Eldefsen, Paul T., Lifson, Jeffrey D., and Picker, Louis J.

Subjects
Immune response -- Research -- Models, Viral vaccines -- Testing -- Research, Genetic vectors -- Testing -- Research -- Models, Simian immunodeficiency virus -- Research -- Development and progression, Virus research -- Research -- Models, Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Cellular immune responses in rhesus macaques (Macaca mulatta) vaccinated with cytomegalovirus vectors expressing SIV proteins are able to stringently control highly pathogenic SIV infection, regardless of the route of challenge, after systemic spread; immunological and virological analyses of protected macaques followed for up to 3 years suggest that persistent immune surveillance by vaccine-elicited immune responses may have cleared the infection. Vaccine combats virulent SIV infection Work on potential vaccines against human immunodeficiency viruses (HIV) and the simian equivalent (SIV) has so far proved largely fruitless. This study makes some progress by exploiting the recent observation that the pathogens appear vulnerable to immune control or pharmacological clearance in the first few hours to days of infection. Rhesus macaques vaccinated with SIV protein-expressing rhesus cytomegalovirus (RhCMV/SIV) vectors developed durable resistance to the highly pathogenic SIVmac239 after challenge by vaginal and intravenous routes. Some of the vaccinated animals have controlled viral replication for 1 to 3 years with no demonstrable evidence for residual virus, raising the possibility that the vaccine- elicited immune responses may in fact have cleared the initial infection. Established infections with the human and simian immunodeficiency viruses (HIV and SIV, respectively) are thought to be permanent with even the most effective immune responses and antiretroviral therapies only able to control, but not clear, these infections.sup.1,2,3,4. Whether the residual virus that maintains these infections is vulnerable to clearance is a question of central importance to the future management of millions of HIV-infected individuals. We recently reported that approximately 50% of rhesus macaques (RM; Macaca mulatta) vaccinated with SIV protein-expressing rhesus cytomegalovirus (RhCMV/SIV) vectors manifest durable, aviraemic control of infection with the highly pathogenic strain SIVmac239 (ref. 5). Here we show that regardless of the route of challenge, RhCMV/SIV vector-elicited immune responses control SIVmac239 after demonstrable lymphatic and haematogenous viral dissemination, and that replication-competent SIV persists in several sites for weeks to months. Over time, however, protected RM lost signs of SIV infection, showing a consistent lack of measurable plasma- or tissue-associated virus using ultrasensitive assays, and a loss of T-cell reactivity to SIV determinants not in the vaccine. Extensive ultrasensitive quantitative PCR and quantitative PCR with reverse transcription analyses of tissues from RhCMV/SIV vector-protected RM necropsied 69-172 weeks after challenge did not detect SIV RNA or DNA sequences above background levels, and replication-competent SIV was not detected in these RM by extensive co-culture analysis of tissues or by adoptive transfer of 60 million haematolymphoid cells to naive RM. These data provide compelling evidence for progressive clearance of a pathogenic lentiviral infection, and suggest that some lentiviral reservoirs may be susceptible to the continuous effector memory T-cell-mediated immune surveillance elicited and maintained by cytomegalovirus vectors., Author(s): Scott G. Hansen [sup.1] , Michael Piatak Jr [sup.2] , Abigail B. Ventura [sup.1] , Colette M. Hughes [sup.1] , Roxanne M. Gilbride [sup.1] , Julia C. Ford [sup.1] [...]

Published
2013
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41. Interleukin-15 response signature predicts RhCMV/SIV vaccine efficacy

Author

Barrenäs, Fredrik, primary, Hansen, Scott G., additional, Law, Lynn, additional, Driscoll, Connor, additional, Green, Richard R., additional, Smith, Elise, additional, Chang, Jean, additional, Golez, Inah, additional, Urion, Taryn, additional, Peng, Xinxia, additional, Whitmore, Leanne, additional, Newhouse, Daniel, additional, Hughes, Colette M., additional, Morrow, David, additional, Randall, Kurt T., additional, Selseth, Andrea N., additional, Ford, Julia C., additional, Gilbride, Roxanne M., additional, Randall, Bryan E., additional, Ainslie, Emily, additional, Oswald, Kelli, additional, Shoemaker, Rebecca, additional, Fast, Randy, additional, Bosche, William J., additional, Axthelm, Michael K., additional, Fukazawa, Yoshinori, additional, Pavlakis, George N., additional, Felber, Barbara K., additional, Fourati, Slim, additional, Sekaly, Rafick-Pierre, additional, Lifson, Jeffrey D., additional, Komorowski, Jan, additional, Kosmider, Ewelina, additional, Shao, Danica, additional, Song, Wenjun, additional, Edlefsen, Paul T., additional, Picker, Louis J., additional, and Gale, Michael, additional

Published
2021
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42. Interleukin-15 response signature predicts RhCMV/SIV vaccine efficacy

Author

Barrenäs, Fredrik, Hansen, Scott G., Law, Lynn, Driscoll, Connor, Green, Richard R., Smith, Elise, Chang, Jean, Golez, Inah, Urion, Taryn, Peng, Xinxia, Whitmore, Leanne, Newhouse, Daniel, Hughes, Colette M., Morrow, David, Randall, Kurt T., Selseth, Andrea N., Ford, Julia C., Gilbride, Roxanne M., Randall, Bryan E., Ainslie, Emily, Oswald, Kelli, Shoemaker, Rebecca, Fast, Randy, Bosche, William J., Axthelm, Michael K., Fukazawa, Yoshinori, Pavlakis, George N., Felber, Barbara K., Fourati, Slim, Sekaly, Rafick-Pierre, Lifson, Jeffrey D., Komorowski, Jan, Kosmider, Ewelina, Shao, Danica, Song, Wenjun, Edlefsen, Paul T., Picker, Louis J., Gale, Michael, Jr., Barrenäs, Fredrik, Hansen, Scott G., Law, Lynn, Driscoll, Connor, Green, Richard R., Smith, Elise, Chang, Jean, Golez, Inah, Urion, Taryn, Peng, Xinxia, Whitmore, Leanne, Newhouse, Daniel, Hughes, Colette M., Morrow, David, Randall, Kurt T., Selseth, Andrea N., Ford, Julia C., Gilbride, Roxanne M., Randall, Bryan E., Ainslie, Emily, Oswald, Kelli, Shoemaker, Rebecca, Fast, Randy, Bosche, William J., Axthelm, Michael K., Fukazawa, Yoshinori, Pavlakis, George N., Felber, Barbara K., Fourati, Slim, Sekaly, Rafick-Pierre, Lifson, Jeffrey D., Komorowski, Jan, Kosmider, Ewelina, Shao, Danica, Song, Wenjun, Edlefsen, Paul T., Picker, Louis J., and Gale, Michael, Jr.

Abstract

Simian immunodeficiency virus (SIV) challenge of rhesus macaques (RMs) vaccinated with strain 68-1 Rhesus Cytomegalovirus (RhCMV) vectors expressing SIV proteins (RhCMV/SIV) results in a binary outcome: stringent control and subsequent clearance of highly pathogenic SIV in similar to 55% of vaccinated RMs with no protection in the remaining 45%. Although previous work indicates that unconventionally restricted, SIV-specific, effector-memory (EM)-biased CD8(+) T cell responses are necessary for efficacy, the magnitude of these responses does not predict efficacy, and the basis of protection vs. non-protection in 68-1 RhCMV/SIV vector-vaccinated RMs has not been elucidated. Here, we report that 68-1 RhCMV/SIV vector administration strikingly alters the whole blood transcriptome of vaccinated RMs, with the sustained induction of specific immune-related pathways, including immune cell, toll-like receptor (TLR), inflammasome/cell death, and interleukin-15 (IL-15) signaling, significantly correlating with subsequent vaccine efficacy. Treatment of a separate RM cohort with IL-15 confirmed the central involvement of this cytokine in the protection signature, linking the major innate and adaptive immune gene expression networks that correlate with RhCMV/SIV vaccine efficacy. This change-from-baseline IL-15 response signature was also demonstrated to significantly correlate with vaccine efficacy in an independent validation cohort of vaccinated and challenged RMs. The differential IL-15 gene set response to vaccination strongly correlated with the pre-vaccination activity of this pathway, with reduced baseline expression of IL-15 response genes significantly correlating with higher vaccine-induced induction of IL-15 signaling and subsequent vaccine protection, suggesting that a robust de novo vaccine-induced IL-15 signaling response is needed to program vaccine efficacy. Thus, the RhCMV/SIV vaccine imparts a coordinated and persistent induction of innate and adaptive immune p

Published
2021
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43. Lymph node T cell responses predict the efficacy of live attenuated SIV vaccines

Author

Fukazawa, Yoshinori, Park, Haesun, Cameron, Mark J., Lefebvre, Francois, Lum, Richard, Coombes, Noel, Mahyari, Eisa, Hagen, Shoko I., Bae, Jin Young, Reyes, III, Marcelo Delos, Swanson, Tonya, Legasse, Alfred W., Sylwester, Andrew, Hansen, Scott G., Smith, Andrew T., Stafova, Petra, Shoemaker, Rebecca, Li, Yuan, Oswald, Kelli, Axthelm, Michael K., McDermott, Adrian, Ferrari, Guido, Montefiori, David C., Edlefsen, Paul T., Piatak, Jr., Michael, Lifson, Jeffrey D., Sekaly, Rafick P., and Picker, Louis J.

Subjects
T cells -- Protection and preservation -- Health aspects -- Physiological aspects -- Genetic aspects -- Research, Simian immunodeficiency virus -- Development and progression -- Protection and preservation -- Health aspects -- Physiological aspects -- Genetic aspects -- Research, AIDS vaccines -- Protection and preservation -- Health aspects -- Physiological aspects -- Genetic aspects -- Research, Biological sciences, Health
Abstract

Live attenuated simian immunodeficiency virus (SIV) vaccines (LAVs) remain the most efficacious of all vaccines in nonhuman primate models of HIV and AIDS, yet the basis of their robust protection remains poorly understood. Here we show that the degree of LAV-mediated protection against intravenous wild-type SIVmac239 challenge strongly correlates with the magnitude and function of SIV-specific, effector-differentiated T cells in the lymph node but not with the responses of such T cells in the blood or with other cellular, humoral and innate immune parameters. We found that maintenance of protective T cell responses is associated with persistent LAV replication in the lymph node, which occurs almost exclusively in follicular helper T cells. Thus, effective LAVs maintain lymphoid tissue-based, effector-differentiated, SIV-specific T cells that intercept and suppress early wild-type SIV amplification and, if present in sufficient frequencies, can completely control and perhaps clear infection, an observation that provides a rationale for the development of safe, persistent vectors that can elicit and maintain such responses., It has been two decades since the first report that LAV administration can completely protect rhesus macaques from subsequent challenge with highly pathogenic, wild-type SIV(1), a degree of efficacy that [...]

Published
2012
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44. Profound early control of highly pathogenic SIV by an effector memory T-cell vaccine

Author

Hansen, Scott G., Ford, Julia C., Lewis, Matthew S., Ventura, Abigail B., Hughes, Colette M., Coyne-Johnson, Lia, Whizin, Nathan, Oswald, Kelli, Shoemaker, Rebecca, Swanson, Tonya, Legasse, Alfred W., Chiuchiolo, Maria J., Parks, Christopher L., Axthelm, Michael K., Nelson, Jay A., Jarvis, Michael A., Piatak, Michael, Lifson, Jeffrey D., and Picker, Louis J.

Published
2011
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47. Mitigation of endemic GI-tract pathogen-mediated inflammation through development of multimodal treatment regimen and its impact on SIV acquisition in rhesus macaques

Author

Bochart, Rachele M., primary, Busman-Sahay, Kathleen, additional, Bondoc, Stephen, additional, Morrow, David W., additional, Ortiz, Alexandra M., additional, Fennessey, Christine M., additional, Fischer, Miranda B., additional, Shiel, Oriene, additional, Swanson, Tonya, additional, Shriver-Munsch, Christine M., additional, Crank, Hugh B., additional, Armantrout, Kimberly M., additional, Barber-Axthelm, Aaron M., additional, Langner, Charlotte, additional, Moats, Cassandra R., additional, Labriola, Caralyn S., additional, MacAllister, Rhonda, additional, Axthelm, Michael K., additional, Brenchley, Jason M., additional, Keele, Brandon F., additional, Estes, Jacob D., additional, Hansen, Scott G., additional, and Smedley, Jeremy V., additional

Published
2021
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48. Modulation of MHC-E transport by viral decoy ligands is required for RhCMV/SIV vaccine efficacy

Author

Verweij, Marieke C., primary, Hansen, Scott G., additional, Iyer, Ravi, additional, John, Nessy, additional, Malouli, Daniel, additional, Morrow, David, additional, Scholz, Isabel, additional, Womack, Jennie, additional, Abdulhaqq, Shaheed, additional, Gilbride, Roxanne M., additional, Hughes, Colette M., additional, Ventura, Abigail B., additional, Ford, Julia C., additional, Selseth, Andrea N., additional, Oswald, Kelli, additional, Shoemaker, Rebecca, additional, Berkemeier, Brian, additional, Bosche, William J., additional, Hull, Michael, additional, Shao, Jason, additional, Sacha, Jonah B., additional, Axthelm, Michael K., additional, Edlefsen, Paul T., additional, Lifson, Jeffrey D., additional, Picker, Louis J., additional, and Früh, Klaus, additional

Published
2021
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49. Myeloid cell tropism enables MHC-E–restricted CD8+ T cell priming and vaccine efficacy by the RhCMV/SIV vaccine.

Author

Hansen, Scott G., Hancock, Meaghan H., Malouli, Daniel, Marshall, Emily E., Hughes, Colette M., Randall, Kurt T., Morrow, David, Ford, Julia C., Gilbride, Roxanne M., Selseth, Andrea N., Trethewy, Renee Espinosa, Bishop, Lindsey M., Oswald, Kelli, Shoemaker, Rebecca, Berkemeier, Brian, Bosche, William J., Hull, Michael, Silipino, Lorna, Nekorchuk, Michael, and Busman-Sahay, Kathleen

Abstract

The strain 68-1 rhesus cytomegalovirus (RhCMV)–based vaccine for simian immunodeficiency virus (SIV) can stringently protect rhesus macaques (RMs) from SIV challenge by arresting viral replication early in primary infection. This vaccine elicits unconventional SIV-specific CD8+ T cells that recognize epitopes presented by major histocompatibility complex (MHC)–II and MHC-E instead of MHC-Ia. Although RhCMV/SIV vaccines based on strains that only elicit MHC-II– and/or MHC-Ia–restricted CD8+ T cells do not protect against SIV, it remains unclear whether MHC-E–restricted T cells are directly responsible for protection and whether these responses can be separated from the MHC-II–restricted component. Using host microRNA (miR)–mediated vector tropism restriction, we show that the priming of MHC-II and MHC-E epitope–targeted responses depended on vector infection of different nonoverlapping cell types in RMs. Selective inhibition of RhCMV infection in myeloid cells with miR-142–mediated tropism restriction eliminated MHC-E epitope–targeted CD8+ T cell priming, yielding an exclusively MHC-II epitope–targeted response. Inhibition with the endothelial cell–selective miR-126 eliminated MHC-II epitope–targeted CD8+ T cell priming, yielding an exclusively MHC-E epitope–targeted response. Dual miR-142 + miR-126–mediated tropism restriction reverted CD8+ T cell responses back to conventional MHC-Ia epitope targeting. Although the magnitude and differentiation state of these CD8+ T cell responses were generally similar, only the vectors programmed to elicit MHC-E–restricted CD8+ T cell responses provided protection against SIV challenge, directly demonstrating the essential role of these responses in RhCMV/SIV vaccine efficacy. RhCMV tropism determines unconventional response: CMV-based vaccine vectors for simian immunodeficiency virus (RhCMV/SIV) lead to profound protection against SIV in rhesus macaques (RMs). This protection is related to the induction of MHC-II– and MHC-E–targeting CD8+ T cells, but it is unclear how these unconventional cells are primed and which are needed for protection. Here, Hansen et al. used microRNAs to limit the ability of RhCMV/SIV vectors to replicate in various cell types. They found that limiting RhCMV/SIV vaccine replication in myeloid cells abrogated the induction of MHC-E–restricted T cells and protection against SIV of in RMs. These data suggest that the unconventional, MHC-E–restricted CD8+ T cells induced by RhCMV/SIV are critical for protection against SIV. [ABSTRACT FROM AUTHOR]

Published
2022
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50. CD8+ T cells fail to limit SIV reactivation following ART withdrawal until after viral amplification

Author

Okoye, Afam A., primary, Duell, Derick D., additional, Fukazawa, Yoshinori, additional, Varco-Merth, Benjamin, additional, Marenco, Alejandra, additional, Behrens, Hannah, additional, Chaunzwa, Morgan, additional, Selseth, Andrea N., additional, Gilbride, Roxanne M., additional, Shao, Jason, additional, Edlefsen, Paul T., additional, Geleziunas, Romas, additional, Pinkevych, Mykola, additional, Davenport, Miles P., additional, Busman-Sahay, Kathleen, additional, Nekorchuk, Michael, additional, Park, Haesun, additional, Smedley, Jeremy, additional, Axthelm, Michael K., additional, Estes, Jacob D., additional, Hansen, Scott G., additional, Keele, Brandon F., additional, Lifson, Jeffery D., additional, and Picker, Louis J., additional

Published
2021
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