Antigen persistence and the control of local T cell memory by migrant respiratory dendritic cells after acute virus infection

Kim, Taeg S.; Hufford, Matthew M.; Sun, Jie; Fu, Yang–Xin; Braciale, Thomas J.

doi:10.1084/jem.20092017

Cited by 172 publications

(189 citation statements)

References 41 publications

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“…It is thus tempting to speculate that the capability of CD8 + T cells to respond to a short Ag pulse might reflect transient viral gene transcription and its preferred feeding of the class I pathway. The fact that CD4 + T cells respond much longer to residual Ag following viral clearance than CD8 + T cells do also indicates that antiviral CD8 + T cell responses depend on viral transcription (79,80).…”

Section: Discussionmentioning

confidence: 99%

Differential Kinetics of Antigen Dependency of CD4+ and CD8+ T Cells

Rabenstein

Ellwart

et al. 2014

The Journal of Immunology

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Ag recognition via the TCR is necessary for the expansion of specific T cells that then contribute to adaptive immunity as effector and memory cells. Because CD4+ and CD8+ T cells differ in terms of their priming APCs and MHC ligands we compared their requirements of Ag persistence during their expansion phase side by side. Proliferation and effector differentiation of TCR transgenic and polyclonal mouse T cells were thus analyzed after transient and continuous TCR signals. Following equally strong stimulation, CD4+ T cell proliferation depended on prolonged Ag presence, whereas CD8+ T cells were able to divide and differentiate into effector cells despite discontinued Ag presentation. CD4+ T cell proliferation was neither affected by Th lineage or memory differentiation nor blocked by coinhibitory signals or missing inflammatory stimuli. Continued CD8+ T cell proliferation was truly independent of self-peptide/MHC-derived signals. The subset divergence was also illustrated by surprisingly broad transcriptional differences supporting a stronger propensity of CD8+ T cells to programmed expansion. These T cell data indicate an intrinsic difference between CD4+ and CD8+ T cells regarding the processing of TCR signals for proliferation. We also found that the presentation of a MHC class II–restricted peptide is more efficiently prolonged by dendritic cell activation in vivo than a class I bound one. In summary, our data demonstrate that CD4+ T cells require continuous stimulation for clonal expansion, whereas CD8+ T cells can divide following a much shorter TCR signal.

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Section: Discussionmentioning

confidence: 99%

Differential Kinetics of Antigen Dependency of CD4+ and CD8+ T Cells

Rabenstein

Ellwart

et al. 2014

The Journal of Immunology

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“…It has been reasonably assumed that the genetic information of the virus is somehow preserved in the host, and its continued expression at a low level is responsible for this persistence. Indeed, viral transcripts have now been detected long after the virus has been cleared; nonetheless, the antigen appears to persist immunologically even longer after such transcripts cease to be detectable (8). Thus, the molecular basis of antigen persistence has remained mysterious.…”

Section: Discussionmentioning

confidence: 99%

“…This is true for chronically infecting viruses, such as the respiratory syncytial (1,2) and Sendai viruses (3), as well as lytic influenza viruses (4)(5)(6)(7)(8). The evidence that antigens persist comes from immunologic rather than biochemical studies: typically, it has been shown by the ability of the host, which has cleared the infection and in which no antigen is detectable, to readily support stimulation of adoptively transferred naïve T cells for weeks after the infection has been cleared.…”

mentioning

confidence: 99%

“…An understanding of the mechanisms of antigen persistence can shed light on several significant immunologic processes: persistence of high levels of viral antigen has been implicated in compromised immune responses to chronic infections. Additionally, antigen persistence has been linked with the nature of T-cell memory elicited in response to infection (4)(5)(6)(7)(8)(9).…”

mentioning

confidence: 99%

“…Indeed, viral transcripts have been detected long after the virus has been cleared; nonetheless, the antigen appears to persist immunologically significantly even longer after such transcripts cease to be detectable (8). Although the idea that antigen persistence is accounted for by undetectable levels of viral DNA or RNA is plausible, it is intellectually unsatisfactory.…”

mentioning

confidence: 99%

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Dendritic cells sequester antigenic epitopes for prolonged periods in the absence of antigen-encoding genetic information

Buckwalter

Basu

et al. 2012

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

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Studies with a number of viral systems have shown, on the basis of the ability of a host to prime naïve T cells, that viral antigens persist in the infected host well beyond complete clearance of the infection and even when viral antigen is undetectable by the most sensitive methods. This has led to a reasonable assumption that the antigen persists through persistence of antigen-encoding genetic information (DNA or RNA) that resides in the host at a subdetectable level. Here, we demonstrate that epitopes, or epitope precursors, of a model antigen (ovalbumin) persist in a host for prolonged periods (weeks), well beyond the time at which the intact antigen has disappeared, and in the complete absence of genetic information encoding it. Dendritic cells are shown to be the site of this epitope sequestration in vivo, as well as in cultures in vitro. For sequestration to occur, the uptaken antigen must be significantly large, that is, the epitope and its 18-mer precursor are not sequestered. Dendritic cells are shown to create an hsp90-dependent intracellular pool of epitopes or epitope precursors that continues to release epitopes for presentation on the major histocompatibility complex I molecules for prolonged periods. Demonstration of such long-term sequestration of antigenic epitopes inside dendritic cells presents new opportunities for stimulation of immune response against cancers and viruses.chaperone | cross-presentation | heat shock protein

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Implantable Silk Composite Microneedles for Programmable Vaccine Release Kinetics and Enhanced Immunogenicity in Transcutaneous Immunization

DeMuth

Min

Irvine

et al. 2013

Adv Healthcare Materials

143

110

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Microneedle vaccines mimic several aspects of cutaneous pathogen invasion by targeting antigen to skin-resident dendritic cells and triggering local inflammatory responses in the skin, which are correlated with enhanced immune responses. Here we tested whether control over vaccine delivery kinetics can enhance immunity through further mimicry of kinetic profiles present during natural acute infections. We report an approach for the fabrication of silk/poly(acrylic acid) (PAA) composite microneedles composed of a silk tip supported on a PAA base. On brief application of microneedle patches to skin, the PAA bases rapidly dissolved to deliver a protein subunit vaccine bolus, while also implanting persistent silk hydrogel depots into the skin for a low-level sustained cutaneous vaccine release over 1-2 weeks. Use of this platform to deliver a model whole-protein vaccine with optimized release kinetics resulted in >10-fold increases in antigen-specific T-cell and humoral immune responses relative to traditional parenteral needle-based immunization.

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Antigen persistence and the control of local T cell memory by migrant respiratory dendritic cells after acute virus infection

Cited by 172 publications

References 41 publications

Differential Kinetics of Antigen Dependency of CD4+ and CD8+ T Cells

Differential Kinetics of Antigen Dependency of CD4+ and CD8+ T Cells

Dendritic cells sequester antigenic epitopes for prolonged periods in the absence of antigen-encoding genetic information

Implantable Silk Composite Microneedles for Programmable Vaccine Release Kinetics and Enhanced Immunogenicity in Transcutaneous Immunization

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