IL-27 is required for shaping the magnitude, affinity distribution, and memory of T cells responding to subunit immunization

Pennock, Nathan D.; Gapin, Laurent; Kedl, Ross M.

doi:10.1073/pnas.1407393111

Cited by 54 publications

(85 citation statements)

References 59 publications

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“…One possibility may be through Program Death-1/Program Death Ligand 1 (PD-1/PD-L1) signaling, because populations of T cells deficient in PD-1 expand more and have higher-avidity TCRs (Jiang et al, 2016). Another factor may be levels of interleukin (IL) 27, a cytokine that is produced by APCs and has been shown to play a role in the generation of high-avidity T cells (Pennock et al, 2014). Similarly, IL-12 produced by dendritic cells may also contribute to the generation of these cells (DeBenedette et al, 2008).…”

Section: Discussionmentioning

confidence: 99%

Distinct Graft-Specific TCR Avidity Profiles during Acute Rejection and Tolerance

et al. 2018

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SUMMARY Mechanisms implicated in robust transplantation tolerance at the cellular level can be broadly categorized into those that inhibit alloreactive T cells intrinsically (clonal deletion and dysfunction) or extrinsically through regulation. Here, we investigated whether additional population-level mechanisms control T cells by examining whether therapeutically induced peripheral transplantation tolerance could influence T cell populations’ avidity for alloantigens. Whereas T cells with high avidity preferentially accumulated during acute rejection of allografts, the alloreactive T cells in tolerant recipients retained a low-avidity profile, comparable to naive mice despite evidence of activation. These contrasting avidity profiles upon productive versus tolerogenic stimulation were durable and persisted upon alloantigen reencounter in the absence of any immunosuppression. Thus, peripheral transplantation tolerance involves control of alloreactive T cells at the population level, in addition to the individual cell level. Controlling expansion or eliminating high-affinity, donorspecific T cells long term may be desirable to achieve robust transplantation tolerance in the clinic.

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Section: Discussionmentioning

confidence: 99%

Distinct Graft-Specific TCR Avidity Profiles during Acute Rejection and Tolerance

et al. 2018

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“…However, there are models in which even outside the competitive setting, IL-27 is required for optimal CD8 + T cell responses (60). A major advance in this area has been the finding that the ability of vaccines that include an adjuvant composed of agonistic anti-CD40 antibodies combined with TLR ligands to elicit CD4 + and CD8 + T cell responses depends on the ability of IL-27 to promote T cell survival (116). These studies are notable because in parallel experiments the authors have shown that IL-27 limits infection-induced CD8 + T cell responses.…”

Section: Il-27 Promotes T Cell Responsesmentioning

confidence: 99%

The Immunobiology of Interleukin-27

Yoshida

Hunter

2015

Annu. Rev. Immunol.

349

433

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Interleukin-27 (IL-27) is a cytokine with strikingly diverse influences on the immune response. Although it was initially linked with the development of Th1 responses, it is now recognized as a potent antagonist of different classes of inflammation through its ability to directly modify CD4(+) and CD8(+) T cell effector functions, to induce IL-10, and to promote specialized T regulatory cell responses. Although this aspect of IL-27 biology has provided insights into how the immune system prevents hyperactivity in the setting of infectious and autoimmune inflammation, in vaccination and cancer models the stimulatory effects of IL-27 on CD8(+) T cell function appear prominent. Additionally, associations between IL-27 and antibody-mediated disease have led to an interest in defining the impact of IL-27 on innate immunity and humoral responses in different disease states. The maturation of this literature has been accompanied by attempts to translate these findings from experimental models into human diseases and by efforts to define where IL-27 might represent a viable therapeutic target.

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“…To date, there are only a few subunit vaccine platforms capable of producing this level of T cell expansion, one of which is a combination adjuvant stimulating both an innate receptor (such as a TLR) and CD40 (combined innate/CD40). Much like the B cell response, the use of either of these single adjuvants typically produces around 10–50,000 total antigen specific CD8+ T cells [2], a number that is non-protective with respect to T cell responses [13]. In contrast, after a single exposure, the combined innate/CD40 adjuvant can produce a similar number of antigen specific T cells (~1–3 million antigen specific T cells), and in the same time frame (7 days), as the infectious challenge [2, 10, 13, 44, 45].…”

Section: T Cell Vs B Cell Fauna… All About the Numbersmentioning

confidence: 99%

“…Much like the B cell response, the use of either of these single adjuvants typically produces around 10–50,000 total antigen specific CD8+ T cells [2], a number that is non-protective with respect to T cell responses [13]. In contrast, after a single exposure, the combined innate/CD40 adjuvant can produce a similar number of antigen specific T cells (~1–3 million antigen specific T cells), and in the same time frame (7 days), as the infectious challenge [2, 10, 13, 44, 45]. As a result of the potency of this vaccine adjuvant, we and others [46–48] have spent years studying its underlying mechanisms in mice and have recently shown its capacity to produce robust CD8 and CD4 responses in non-human primates [49].…”

Section: T Cell Vs B Cell Fauna… All About the Numbersmentioning

confidence: 99%

“…While infectious models have shown central roles for type I IFN and IL-12 for mediating T cell differentiation and memory formation, these cytokines are often dispensable in the T cell response to subunit vaccination [1]. In contrast, IL-27 signaling appears to be required for the T cell responses to a host of subunit adjuvants [2], while the response to infectious challenge is either unaffected or even elevated in the absence of this cytokine [3, 4]. TNF receptor superfamily members expressed by T cells largely enhance various qualitative aspects of the T cell responses during infection [5–8], but instead dictate the quantitative magnitude of the response in subunit vaccine settings [9–15].…”

Section: Introductionmentioning

confidence: 99%

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T Cell Vaccinology: Beyond the Reflection of Infectious Responses

Pennock

Kedl

2016

Trends in Immunology

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Inducing sustained, robust CD8+ T cell responses is necessary for therapeutic intervention in chronic infectious diseases and cancer. Unfortunately, most adjuvant formulations fail to induce substantial cellular immunity in humans. Attenuated acute infectious agents induce strong CD8+ T cell immunity, and are thought to therefore represent a good road map for guiding the development of subunit vaccines capable of inducing the same. However, recent evidence suggests that this assumption may need reconsideration. Here we provide an overview of subunit vaccine history as it pertains to instigating T cell responses. We argue that in light of evidence demonstrating that T cell responses to vaccination differ from those induced by infectious challenge, research in pursuit of cellular immunity-inducing vaccine adjuvants should no longer follow only the infection paradigm.

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IL-27 is required for shaping the magnitude, affinity distribution, and memory of T cells responding to subunit immunization

Cited by 54 publications

References 59 publications

Distinct Graft-Specific TCR Avidity Profiles during Acute Rejection and Tolerance

Distinct Graft-Specific TCR Avidity Profiles during Acute Rejection and Tolerance

The Immunobiology of Interleukin-27

T Cell Vaccinology: Beyond the Reflection of Infectious Responses

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