CD8 + T cells specific to a single Yersinia pseudotuberculosis epitope restrict bacterial replication in the liver but fail to provide sterilizing immunity

Shen, Haiqian; Blanchette, Krystle A.; Crimmins, Gregory T.; Bergman, Molly A.; Isberg, Ralph R.; Orihuela, Carlos J.; Dube, Peter H.

doi:10.1016/j.meegid.2016.06.008

Cited by 3 publications

(10 citation statements)

References 41 publications

(48 reference statements)

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“…Female and male C57BL/6 mice vaccinated with 2 × 10 4 CFU of the OVA-expressing L. monocytogenes strain developed a robust OVA specific CD8 + /TCRβ + T-cell response while those vaccinated with the parental L. monocytogenes strain did not ( Figure 1B and 1C). As previously reported by us and others [28,29], a single vaccination with increasing doses of Lm: OVA (2 × 10 5 or 2 × 10 6 CFU) vaccine failed to significantly increase the numbers of OVA specific CD8 + /TCRβ + T-cells (Supplementary Figure 1A and 1B). Importantly, the ΔactA:plcB (Lm: Parental) as well as the actA-OVA fusion (Lm: OVA) vaccine strains were completely attenuated with i. v. vaccination doses up to 2 × 10 7 CFU ( Figure 1D).…”

Section: Vaccination With L Monocytogenes Expressing Tumor Antigens supporting

confidence: 84%

“…Although others have reported similar protection with oral or intra-muscular routes of vaccination [29], the safety of this specific strain [26,28] and newer phase I safety trials [45] suggest vaccination via the i.v. route is not a barrier to utilization.…”

Section: Discussionmentioning

confidence: 88%

“…We previously showed that the Lm: OVA vaccine induces a robust antigen-specific CD8 + /TCRβ + T-cell response ( Figure 1B and 1C) and [28]. However, both CD8 + T-cells and NK cells have been shown to be important in Lm vaccine-mediated immunity [36].…”

Section: Cd8 + T-cells Are Responsible For Anti-tumor Immunitymentioning

confidence: 91%

“…We previously described the Listeria monocytogenes strain deficient in both actin-assembly inducing protein (actA) and phospholipase C (plcB) [28], which was used as the vaccine platform in this study. This double mutant is completely attenuated in humans, lacking the ability to directly enter a neighboring cell or escape a secondary membrane [34], and importantly it is unable to cause neuro-invasiveness [35].…”

Section: Vaccination With L Monocytogenes Expressing Tumor Antigens mentioning

confidence: 99%

“…Several Lm cancer vaccination platforms have fused tumorassociated antigens (TAA) to the LLO peptide [22][23][24]. Due to its proinflammatory properties [25] and lack of pathogenesis in human subjects [26], we developed an actA:plcB double mutant with the TAA peptide fused to the first 100 amino acids of ActA [27,28]. Fusing TAAs to ActA results in the TAA being delivered directly to the cytoplasm and thus the MHC-I processing compartment.…”

Section: Introductionmentioning

confidence: 99%

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Checkpoint blockade inhibitors enhances the effectiveness of aListeria monocytogenes-based melanoma vaccine

Gilley

Dube

2020

Oncotarget

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Melanoma continues to be a significant health concern worldwide despite recent improvements in treatment. Unlike many other prominent cancers, melanoma incidence in both men and women increased over the past decade in the U. S. and much of the developed world. The single greatest risk factor for melanoma is damage from ultraviolet radiation associated with lifestyle. The lifestyle component suggests that although melanoma risk can be minimized with behavioral changes, vaccinating highrisk individuals against melanoma may be the most efficacious preventative method. Accordingly, using a highly attenuated, double-mutant L. monocytogenes strain expressing a tumor-associated antigen, we obtained significant protection against melanoma in a mouse model. The Listeria-based vaccine induced protection through antigen-specific CD8+ T-cells inducing both a protective primary and a memory T-cell response. Vaccinated animals were significantly protected from melanoma. When used in conjunction with checkpoint blockade treatment, the vaccine substantially reduced tumor size and number relative to animals receiving checkpoint blockade (CPB) alone. This study provides evidence that CPB treatment synergizes with a L. monocytogenes-based melanoma vaccine to enhance vaccine-mediated protection.

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Section: Vaccination With L Monocytogenes Expressing Tumor Antigens supporting

confidence: 84%

Section: Discussionmentioning

confidence: 88%

Section: Cd8 + T-cells Are Responsible For Anti-tumor Immunitymentioning

confidence: 91%

Section: Vaccination With L Monocytogenes Expressing Tumor Antigens mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Checkpoint blockade inhibitors enhances the effectiveness of aListeria monocytogenes-based melanoma vaccine

Gilley

Dube

2020

Oncotarget

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YopE specific CD8+ T cells provide protection against systemic and mucosal Yersinia pseudotuberculosis infection

et al. 2017

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Prior studies indicated that CD8+ T cells responding to a surrogate single antigen expressed by Y. pseudotuberculosis, ovalbumin, were insufficient to protect against yersiniosis. Herein we tested the hypothesis that CD8+ T cells reactive to the natural Yersinia antigen YopE would be more effective at providing mucosal protection. We first confirmed that immunization with the attenuated ksgA- strain of Y. pseudotuberculosis generated YopE-specific CD8+ T cells. These T cells were protective against challenge with virulent Listeria monocytogenes expressing secreted YopE. Mice immunized with an attenuated L. monocytogenes YopE+ strain generated large numbers of functional YopE-specific CD8+ T cells, and initially controlled a systemic challenge with virulent Y. pseudotuberculosis, yet eventually succumbed to yersiniosis. Mice vaccinated with a YopE peptide and cholera toxin vaccine generated robust T cell responses, providing protection to 60% of the mice challenged mucosally but failed to show complete protection against systemic infection with virulent Y. pseudotuberculosis. These studies demonstrate that vaccination with recombinant YopE vaccines can generate YopE-specific CD8+ T cells, that can provide significant mucosal protection but these cells are insufficient to provide sterilizing immunity against systemic Y. pseudotuberculosis infection. Our studies have implications for Yersinia vaccine development studies.

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Cross-Talk Between Antigen Presenting Cells and T Cells Impacts Intestinal Homeostasis, Bacterial Infections, and Tumorigenesis

2019

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Innate immunity is maintained in part by antigen presenting cells (APCs) including dendritic cells, macrophages, and B cells. APCs interact with T cells to link innate and adaptive immune responses. By displaying bacterial and tumorigenic antigens on their surface via major histocompatibility complexes, APCs can directly influence the differentiation of T cells. Likewise, T cell activation, differentiation, and effector functions are modulated by APCs utilizing multiple mechanisms. The objective of this review is to describe how APCs interact with and influence the activation of T cells to maintain innate immunity during exposure to microbial infection and malignant cells. How bacteria and cancer cells take advantage of some of these interactions for their own benefit will also be discussed. While this review will cover a broad range of topics, a general focus will be held around pathogens, cancers, and interactions that typically occur within the gastrointestinal tract.

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CD8 + T cells specific to a single Yersinia pseudotuberculosis epitope restrict bacterial replication in the liver but fail to provide sterilizing immunity

Cited by 3 publications

References 41 publications

Checkpoint blockade inhibitors enhances the effectiveness of aListeria monocytogenes-based melanoma vaccine

Checkpoint blockade inhibitors enhances the effectiveness of aListeria monocytogenes-based melanoma vaccine

YopE specific CD8+ T cells provide protection against systemic and mucosal Yersinia pseudotuberculosis infection

Cross-Talk Between Antigen Presenting Cells and T Cells Impacts Intestinal Homeostasis, Bacterial Infections, and Tumorigenesis

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