Combinatorial immunotherapeutic approaches to restore the function of anergic tumor-reactive cytotoxic CD8<sup>+</sup> T cells

Redmond, William L.; Linch, Stefanie N.

doi:10.1080/21645515.2016.1193277

Cited by 9 publications

(9 citation statements)

References 45 publications

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“…Our demonstration that an OX40 agonist can tilt the immune response toward HBV clearance in young mice and in adult chronic mice that encountered antigen when they were young opens new avenues for treating CHB in humans. Preclinical studies using tumor models demonstrate that tumorassociated, antigenspecific CD8 + T cells increase in quantity after OX40 agonist immunotherapy, and OX40 agonists, plus and minus checkpoint blockade, lead to reduced tumor growth and improved overall sur vival (25)(26)(27)(28). Our data suggest that the OX40/OX40L pathway is crucial for effective HBV immunity and that OX40 agonists have po tential in definitively treating CHB by augmenting the virusspecific T cell response.…”

Section: Discussionmentioning

confidence: 64%

An OX40/OX40L interaction directs successful immunity to hepatitis B virus

et al. 2018

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Depending on age of acquisition, hepatitis B virus (HBV) can induce a cell-mediated immune response that results in either cure or progressive liver injury. In adult-acquired infection, HBV antigens are usually cleared, whereas in infancy-acquired infection, they persist. Individuals infected during infancy therefore represent the majority of patients chronically infected with HBV (CHB). A therapy that can promote viral antigen clearance in most CHB patients has not been developed and would represent a major health care advance and cost mitigator. Using an age-dependent mouse model of HBV clearance and persistence in conjunction with human blood and liver tissue, we studied mechanisms of viral clearance to identify new therapeutic targets. We demonstrate that age-dependent expression of the costimulatory molecule OX40 ligand (OX40L) by hepatic innate immune cells is pivotal in determining HBV immunity, and that treatment with OX40 agonists leads to improved HBV antigen clearance in young mice, as well as increased strength of T cell responses in young mice and adult mice that were exposed to HBV when they were young and developed a CHB serological profile. Similarly, in humans, we show that hepatic OX40L transcript expression is age-dependent and that increased OX40 expression on peripheral CD4+ T cells in adults is associated with HBV clearance. These findings provide new mechanistic understanding of the immune pathways and cells necessary for HBV immunity and identify potential therapeutic targets for resolving CHB.

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Section: Discussionmentioning

confidence: 64%

An OX40/OX40L interaction directs successful immunity to hepatitis B virus

et al. 2018

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“…Tumor evasive properties are probably fine-tuned to be activated in the wake of a profound T E response which may limit cytolytic functions. Possibly evasive mechanisms include down-regulation of MHC Class I that prevents T E cells from engaging their tumor target [42], the recruitment of regulatory T cells that can directly and indirectly (modulation of cytokine environment) impairs T E function [43] and the up-regulation of checkpoint ligands such as PD-L1 that are known to engage PD-1 on T E cells and interfere with TCR signaling, impairing cytolytic function [44]. Overall, the results of this study highlights the complexity of a two-way cross-regulation between host immunity and a rapidly growing tumor.…”

Section: Discussionmentioning

confidence: 99%

Homologous Prime-Boost Vaccination with OVA Entrapped in Self-Adjuvanting Archaeosomes Induces High Numbers of OVA-Specific CD8+ T Cells that Protect Against Subcutaneous B16-OVA Melanoma

2016

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Homologous prime-boost vaccinations with live vectors typically fail to induce repeated strong CD8+ T cell responses due to the induction of anti-vector immunity, highlighting the need for alternative delivery vehicles. The unique ether lipids of archaea may be constituted into liposomes, archaeosomes, which do not induce anti-carrier responses, making them an ideal candidate for use in repeat vaccination systems. Herein, we evaluated in mice the maximum threshold of antigen-specific CD8+ T cell responses that may be induced by multiple homologous immunizations with ovalbumin (OVA) entrapped in archaeosomes derived from the ether glycerolipids of the archaeon Methanobrevibacter smithii (MS-OVA). Up to three immunizations with MS-OVA administered in optimized intervals (to allow for sufficient resting of the primed cells prior to boosting), induced a potent anti-OVA CD8+ T cell response of up to 45% of all circulating CD8+ T cells. Additional MS-OVA injections did not add any further benefit in increasing the memory of CD8+ T cell frequency. In contrast, OVA expressed by Listeria monocytogenes (LM-OVA), an intracellular bacterial vector failed to evoke a boosting effect after the second injection, resulting in significantly reduced antigen-specific CD8+ T cell frequencies. Furthermore, repeated vaccination with MS-OVA skewed the response increasingly towards an effector memory (CD62low) phenotype. Vaccinated animals were challenged with B16-OVA at late time points after vaccination (+7 months) and were afforded protection compared to control. Therefore, archaeosomes constituted a robust particulate delivery system to unravel the kinetics of CD8+ T cell response induction and memory maintenance and constitute an efficient vaccination regimen optimized for tumor protection.

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“…Highly immunogenic tumor-derived neo-epitopes must be present to be recognized by cytotoxic T cells. Antigen (Ag)-loaded dendritic cells (DCs) are the most commonly used cell-based vaccines with proven safety and, notably, the capability of providing long-lasting protective immunity [ 2 – 4 ]. As such, vaccines hold promise to delay or prevent cancer recurrence, particularly in early-stage disease patients, when immune-suppressive mechanisms are not firmly established.…”

Section: Introductionmentioning

confidence: 99%

In vivo vaccination with cell line-derived whole tumor lysates: neoantigen quality, not quantity matters

et al. 2020

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Background Cancer vaccines provide a complex source of neoantigens. Still, increasing evidence reveals that the neoantigen quality rather than the quantity is predictive for treatment outcome. Methods Using the preclinical Mlh1−/− tumor model, we performed a side-by side comparison of two autologous cell-line derived tumor lysates (namely 328 and A7450 T1 M1) harboring different tumor mutational burden (TMB; i.e. ultra-high: 328; moderate-high: A7450 T1 M1). Mice received repetitive prophylactic or therapeutic applications of the vaccine. Tumor incidence, immune responses and tumor microenvironment was examined. Results Both tumor cell lysates delayed tumor formation in the prophylactic setting, with the A7450 T1 M1 lysate being more effective in decelerating tumor growth than the 328 lysate (median overall survival: 37 vs. 25 weeks). Comparable results were achieved in therapeutic setting and could be traced back to antigen-driven immune stimulation. Reactive T cells isolated from A7450 T1 M1-treated mice recognized autologous Mlh1−/− tumor cells in IFNγ ELISpot, but likewise YAC-1 cells, indicative for stimulation of both arms of the immune system. By deciphering local effects, vaccines shaped the tumor microenvironment differently. While A7450 T1 M1 prophylactically vaccinated tumors harbored low numbers of myeloid-derived suppressor cells (MDSC) and elevated CD8-T cell infiltrates, vaccination with the 328 lysate evoked MDSC infiltration. Similar effects were seen in the therapeutic setting with stable disease induction only upon A7450 T1 M1 vaccination. Untangling individual response profiles revealed strong infiltration with LAG3+ and PD-L1+ immune cells when treatments failed, but almost complete exclusion of checkpoint-expressing lymphocytes in long-term survivors. Conclusions By applying two tumor cell lysates we demonstrate that neoantigen quality outranks quantity. This should be considered prior to designing cancer vaccine-based combination approaches.

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Combinatorial immunotherapeutic approaches to restore the function of anergic tumor-reactive cytotoxic CD8⁺ T cells

Cited by 9 publications

References 45 publications

An OX40/OX40L interaction directs successful immunity to hepatitis B virus

An OX40/OX40L interaction directs successful immunity to hepatitis B virus

Homologous Prime-Boost Vaccination with OVA Entrapped in Self-Adjuvanting Archaeosomes Induces High Numbers of OVA-Specific CD8+ T Cells that Protect Against Subcutaneous B16-OVA Melanoma

In vivo vaccination with cell line-derived whole tumor lysates: neoantigen quality, not quantity matters

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Combinatorial immunotherapeutic approaches to restore the function of anergic tumor-reactive cytotoxic CD8+ T cells

Cited by 9 publications

References 45 publications

An OX40/OX40L interaction directs successful immunity to hepatitis B virus

An OX40/OX40L interaction directs successful immunity to hepatitis B virus

Homologous Prime-Boost Vaccination with OVA Entrapped in Self-Adjuvanting Archaeosomes Induces High Numbers of OVA-Specific CD8+ T Cells that Protect Against Subcutaneous B16-OVA Melanoma

In vivo vaccination with cell line-derived whole tumor lysates: neoantigen quality, not quantity matters

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Combinatorial immunotherapeutic approaches to restore the function of anergic tumor-reactive cytotoxic CD8⁺ T cells