Preclinical efficacy of immune-checkpoint monotherapy does not recapitulate corresponding biomarkers-based clinical predictions in glioblastoma

Garg, Abhishek D.; Vandenberk, Lien; Woensel, Matthias Van; Belmans, Jochen; Schaaf, Marco B.E.; Boon, Louis; Vleeschouwer, Steven De; Agostinis, Patrizia

doi:10.1080/2162402x.2017.1295903

Cited by 56 publications

(61 citation statements)

References 64 publications

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“…Further studies will be needed to determine whether therapeutic drug combinations to manipulate these factors will, in turn, directly impact intratumoral immune cytolytic activity and lead to an immune-mediated anti-tumor effect. Consistent with other studies [7,27,35], we found no association between the non-synonymous TMB and the degree of intratumoral immune cytolytic activity in GBM.…”

Section: Discussionsupporting

confidence: 92%

RNA-seq for identification of therapeutically targetable determinants of immune activation in human glioblastoma

et al. 2018

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Introduction: We sought to determine which therapeutically targetable immune checkpoints, costimulatory signals, and other tumor microenvironment (TME) factors are independently associated with immune cytolytic activity (CYT), a gene expression signature of activated effector T cells, in human glioblastoma (GBM). Methods: GlioVis was accessed for RNA-seq data from The Cancer Genome Atlas (TCGA). For subjects with treatment-naïve, primary GBM, we quantified mRNA expression of 28 therapeutically targetable TME factors. CYT (geometric mean of GZMA and PRF1 expression) was calculated for each tumor. Multiple linear regression was performed to determine the relationship between the dependent variable (CYT) and mRNA expression of each of the 28 factors. Variables associated with CYT in multivariate analysis were subsequently evaluated for this association in an independent cohort of newly diagnosed GBMs from the Chinese Glioma Cooperative Group (CGCG). Results: 109 TCGA tumors were analyzed. The final multiple linear regression model included the following variables, each positively associated with CYT except VEGF-A (negative association): CSF-1 (p=0.003), CD137 (p=0.042), VEGF-A (p<0.001), CTLA4 (p=0.028), CD40 (p=0.023), GITR (p=0.020), IL6 (p=0.02), and OX40 (p<0.001). In CGCG (n=52), each of these variables remained significantly associated with CYT in univariate analysis except for VEGF-A. In multivariate analysis, only CTLA4 and CD40 remained statistically significant. Conclusions: Using multivariate modeling of RNA-seq gene expression data, we identified therapeutically targetable TME factors that are independently associated with intratumoral cytolytic T-cell activity in human GBM. As a myriad of systemic immunotherapies are now available for investigation, our results could inform rational combinations for evaluation in GBM.

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Section: Discussionsupporting

confidence: 92%

RNA-seq for identification of therapeutically targetable determinants of immune activation in human glioblastoma

et al. 2018

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“…1 and Table 1) -a cancer type that appears to be particularly resistant to ICBs but responsive to DC-based vaccines. 184,187,241 Interestingly, recombinant TAAs, TAA-derived peptides and tumor-cell lysates remain the preferred source of antigens for loading DCs for DC-based vaccines across both published and ongoing clinical studies ( Fig. 1 and Table 1).…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, we analyze the broad impact of cancer immunotherapies including immune checkpoint blockers (ICBs), 179,180 and adoptive T-cell transfer (ACT) 181,182 on the field of DC-based vaccines. 183,184 Indeed, ongoing clinical trials are identifying a niche for DC-based vaccines in a cancer immunotherapy landscape dominated by ICBs and ACT.…”

Section: Introductionmentioning

confidence: 99%

Trial watch: Dendritic cell-based anticancer immunotherapy

et al. 2017

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Dendritic cell (DC)-based vaccines against cancer have been extensively developed over the past two decades. Typically DC-based cancer immunotherapy entails loading patient-derived DCs with an appropriate source of tumor-associated antigens (TAAs) and efficient DC stimulation through a so-called "maturation cocktail" (typically a combination of pro-inflammatory cytokines and Toll-like receptor agonists), followed by DC reintroduction into patients. DC vaccines have been documented to (re)activate tumor-specific T cells in both preclinical and clinical settings. There is considerable clinical interest in combining DC-based anticancer vaccines with T cell-targeting immunotherapies. This reflects the established capacity of DC-based vaccines to generate a pool of TAA-specific effector T cells and facilitate their infiltration into the tumor bed. In this Trial Watch, we survey the latest trends in the preclinical and clinical development of DC-based anticancer therapeutics. We also highlight how the emergence of immune checkpoint blockers and adoptive T-cell transfer-based approaches has modified the clinical niche for DC-based vaccines within the wide cancer immunotherapy landscape.

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“…C or CD8 C T cells, amongst others; [251][252][253] (2) the circulating levels of multiple cytokines, such as interferon, gamma (IFNG; best known as IFN-g), 254 IL6, 255 and tumor necrosis factor (TNF); 256-258 (3) the amounts of TAA-specific T cells (via tetramer assays); 259,260 (4) the tumor mutational load and/or the abundance of predicted neo-antigens (via genome or whole-exome sequencing); 115,138,[261][262][263][264][265] and (5) the levels of circulating biomarkers of ICD (via proteomic or metabolomic assays).…”

Section: Ongoing Clinical Trialsmentioning

confidence: 99%

“…[105][106][107][108][109][110] Accordingly, RCD can no longer be perceived as immunogenic when: (1) the intracellular stress responses regulating the emission of ICD-associated DAMPs are pharmacologically or genetically ablated in cancer cells; or (2) when the molecular machinery dedicated to DAMP detection is inhibited or ablated. 13,44,84,91,93,97 Moreover, ICD-driven immunity can no longer operate in the presence of general immunological defects, 111 such as (1) an intrinsically low antigenicity of cancer cells, owing to low levels of TAAs or downregulation of MHC Class I molecules [112][113][114][115][116][117][118][119] ; (2) an increased immunological tolerance of the host, secondary to increased amounts of immunosuppressive cytokines, [120][121][122][123][124][125][126][127][128] or inhibitors of chemotaxis, [129][130][131][132][133][134] increased tumor infiltration by immunosuppressive cell populations, [135][136][137][138][139][140]…”

Section: Introductionmentioning

confidence: 99%

Trial watch: Immunogenic cell death induction by anticancer chemotherapeutics

et al. 2017

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The expression "immunogenic cell death" (ICD) refers to a functionally unique form of cell death that facilitates (instead of suppressing) a T cell-dependent immune response specific for dead cell-derived antigens. ICD critically relies on the activation of adaptive responses in dying cells, culminating with the exposure or secretion of immunostimulatory molecules commonly referred to as "damage-associated molecular patterns". Only a few agents can elicit bona fide ICD, including some clinically established chemotherapeutics such as doxorubicin, epirubicin, idarubicin, mitoxantrone, bleomycin, bortezomib, cyclophosphamide and oxaliplatin. In this Trial Watch, we discuss recent progress on the development of ICD-inducing chemotherapeutic regimens, focusing on studies that evaluate clinical efficacy in conjunction with immunological biomarkers.

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Preclinical efficacy of immune-checkpoint monotherapy does not recapitulate corresponding biomarkers-based clinical predictions in glioblastoma

Cited by 56 publications

References 64 publications

RNA-seq for identification of therapeutically targetable determinants of immune activation in human glioblastoma

RNA-seq for identification of therapeutically targetable determinants of immune activation in human glioblastoma

Trial watch: Dendritic cell-based anticancer immunotherapy

Trial watch: Immunogenic cell death induction by anticancer chemotherapeutics

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