Immune clearance of highly pathogenic SIV infection

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

doi:10.1038/nature12519

Cited by 561 publications

(621 citation statements)

References 27 publications

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“…However, many persistent viral infections such as CMV and EBV in humans lead to CD8 T-cell responses reaching a higher magnitude than most acute infections. Hansen et al (42,43) have recently reported that rhesus macaques vaccinated with persistent rhesus CMV expression vectors containing simian immunodeficiency virus (SIV) proteins elicit durable viral control after challenge with SIV. The studies suggested that the SIV control was linked to a large magnitude of CD8 T cells generated and maintained by the persistent vector at sites of viral entry (mucosa) and at other sites of potential viral dissemination.…”

Section: Discussionmentioning

confidence: 99%

Initial viral load determines the magnitude of the human CD8 T cell response to yellow fever vaccination

Akondy

Johnson²,

Nakaya

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

108

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CD8 T cells are a potent tool for eliminating intracellular pathogens and tumor cells. Thus, eliciting robust CD8 T-cell immunity is the basis for many vaccines under development. However, the relationship between antigen load and the magnitude of the CD8 T-cell response is not well-described in a human immune response. Here we address this issue by quantifying viral load and the CD8 T-cell response in a cohort of 80 individuals immunized with the live attenuated yellow fever vaccine (YFV-17D) by sampling peripheral blood at days 0, 1, 2, 3, 5, 7, 9, 11, 14, 30, and 90. When the virus load was below a threshold (peak virus load < 225 genomes per mL, or integrated virus load < 400 genome days per mL), the magnitude of the CD8 T-cell response correlated strongly with the virus load (R 2 ∼ 0.63). As the virus load increased above this threshold, the magnitude of the CD8 T-cell responses saturated. Recent advances in CD8 T-cell-based vaccines have focused on replication-incompetent or single-cycle vectors. However, these approaches deliver relatively limited amounts of antigen after immunization. Our results highlight the requirement that T-cellbased vaccines should deliver sufficient antigen during the initial period of the immune response to elicit a large number of CD8 T cells that may be needed for protection.vaccines | human CD8 T cells | viral load | effector T cells | immune memory C D8 T cells provide a powerful mechanism for elimination of intracellular pathogens and tumor cells. Accordingly, a major thrust of current vaccine research focuses on stimulating robust T-cell immunity for defense against infections such as HIV, malaria, tuberculosis, Ebola virus, herpes viruses, and hepatitis C virus (HCV) (1-8). Inducing effective CD8 T-cell immunity is also an important goal for cancer vaccines (9, 10). However, how antigen load affects the CD8 T-cell response has not been quantified in a detailed manner during a human immune response. In this study we address this question using the human live attenuated yellow fever vaccine (YFV-17D) vaccine.The dynamics of CD8 T-cell responses to intracellular infection have been extensively studied in model systems. Infection typically stimulates a rapid burst of proliferation in antigenspecific CD8 T cells with division occurring as quickly as once in 4-6 h (11). This expansion results in a large population of effector CD8 T cells that aid in clearance of infected cells. Although most (90-95%) of the effector CD8 T cells die, a small fraction differentiate to form long-term memory CD8 T cells (12). Detailed quantitative measurements of the dynamics of virus and the CD8 T-cell response to the YFV-17D vaccine allow us to characterize these basic features of the CD8 T-cell responses in humans. Additionally, tracking the dynamics of both virus and CD8 T cells over time in a large cohort allows us to explore the relationship between amount of antigen and the magnitude of expansion and answer the following questions: Is there a threshold amount of virus required to generate a r...

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Section: Discussionmentioning

confidence: 99%

Initial viral load determines the magnitude of the human CD8 T cell response to yellow fever vaccination

Akondy

Johnson²,

Nakaya

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

108

View full text Add to dashboard Cite

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“…Along with the evidence that HIV infections impair the thymic output, this furthermore reveals the retention of T-cells in established chronic infections that can expand substantially 30,31 . The demonstration that virus titers strongly rise following depletion of CD8 + T-cells in SIV infected macaques [32][33][34] and that protective immune responses can be elicited upon vaccinating SIV infected Rhesus macaques 35 further underscore the strong effector capacity of CD8 + T-cells in established chronic infections.…”

Section: Evidence That Functional T-cells Are Maintained In Chronic Imentioning

confidence: 93%

T cell differentiation in chronic infection and cancer: functional adaptation or exhaustion?

et al. 2014

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Chronic viral infections and malignant tumours induce T cells that have a reduced ability to secrete effector cytokines and have upregulated expression of the inhibitory receptor PD1 (programmed cell death protein 1). These features have so far been considered to mark terminally differentiated 'exhausted' T cells. However, several recent clinical and experimental observations indicate that phenotypically exhausted T cells can still mediate a crucial level of pathogen or tumour control. In this Opinion article, we propose that the exhausted phenotype results from a differentiation process in which T cells stably adjust their effector capacity to the needs of chronic infection. We argue that this phenotype is optimized to cause minimal tissue damage while still mediating a critical level of pathogen control. In contrast to the presently held view of functional exhaustion, this new concept better reflects the pathophysiology and clinical manifestations of persisting infections, and it provides a rationale for emerging therapies that enhance T cell activity in chronic infection and cancer by blocking inhibitory receptors. Daniel T. Utzschneider Division of Immunology and Allergy of the Lausanne University Hospital (CHUV) and Swiss Vaccine Research Institute (SVRI), Lausanne, SwitzerlandDaniel Utzschneider is a PhD student of Dietmar Zehn. His research is focused on T-cell differentiation in chronic infection. Susanne G. Oberle Division of Immunology and Allergy of the Lausanne University Hospital (CHUV) and Swiss Vaccine Research Institute (SVRI), Lausanne, SwitzerlandSusanne Oberle is a PhD student of Dietmar Zehn. Her research interests are focused on investigating T-cell responses in acute and chronic infections. and it provides a rational for emerging therapies that enhance T-cell activity in chronic infection and cancer by blocking inhibitory receptors. Christian Münz PhD

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“…A beneficial role for CD8 + T cells in blocking acquisition is less apparent, although this possibility cannot be dismissed. Intriguing studies suggest that CD8 + T-cell responses elicited by a replicating viral vector vaccine can clear a nascent simian immunodeficiency virus (SIV) infection in roughly half of vaccinated nonhuman primates (18). These responses alone did not block acquisition but could contribute to such an effect if combined with certain humoral responses.…”

mentioning

confidence: 99%

Antibody persistence and T-cell balance: Two key factors confronting HIV vaccine development

Lewis

DeVico

Gallo

2014

Proc. Natl. Acad. Sci. U.S.A.

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The quest for a prophylactic AIDS vaccine is ongoing, but it is now clear that the successful vaccine must elicit protective antibody responses. Accordingly, intense efforts are underway to identify immunogens that elicit these responses. Regardless of the mechanism of antibodymediated protection, be it neutralization, Fc-mediated effector function, or both, antibody persistence and appropriate T-cell help are significant problems confronting the development of a successful AIDS vaccine. Here, we discuss the evidence illustrating the poor persistence of antibody responses to Env, the envelope glycoprotein of HIV-1, and the related problem of CD4 + T-cell responses that compromise vaccine efficacy by creating excess cellular targets of HIV-1 infection. Finally, we propose solutions to both problems that are applicable to all Envbased AIDS vaccines regardless of the mechanism of antibody-mediated protection.

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Immune clearance of highly pathogenic SIV infection

Cited by 561 publications

References 27 publications

Initial viral load determines the magnitude of the human CD8 T cell response to yellow fever vaccination

Initial viral load determines the magnitude of the human CD8 T cell response to yellow fever vaccination

T cell differentiation in chronic infection and cancer: functional adaptation or exhaustion?

Antibody persistence and T-cell balance: Two key factors confronting HIV vaccine development

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