Co-stimulatory signaling determines tumor antigen sensitivity and persistence of CAR T cells targeting PSCA+ metastatic prostate cancer

Priceman, Saul J.; Gerdts, Ethan; Tilakawardane, Dileshni; Kennewick, Kelly T.; Murad, John P.; Park, Anthony K.; Jeang, Brook; Yamaguchi, Yukiko; Yang, Xin; Urak, Ryan; Weng, Lihong; Chang, Wen-Chung; Wright, Sarah; Pal, Sumanta K.; Reiter, Robert E.; Wu, Anna M.; Brown, Christine E.; Forman, Stephen J.

doi:10.1080/2162402x.2017.1380764

Cited by 133 publications

(165 citation statements)

References 45 publications

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“…87 Similarly, PSCA-directed CARs utilizing a 4-1BB costimulatory domain demonstrated activity only in response to cells expressing high levels of the antigen, whereas CARs utilizing a CD28 costimulatory domain were able to target cells expressing either high or low levels of the PSCA antigen. 37 Interestingly, these findings correlate with the kinetics of CAR T cell responses in vivo which may reflect the relative sensitivity of each CAR. 88 As these findings are currently limited to a few models, further studies are needed to determine if these findings are generalizable to all CAR constructs and how this can be incorporated into CAR T cell therapy to reduce the occurrence of antigen low relapse.…”

Section: Role Of Car Structure In Antigen Sensitivitymentioning

confidence: 83%

“…Each of these costimulatory domains have proven sufficient in promoting effective CAR T cell responses in vivo in various preclinical models and clinical trials, however, the incorporation of the 4-1BB domain has demonstrated a significant impact on the in vivo persistence of CAR T cells. 34,36,37 This has been most notable when comparing CAR T cells targeting CD19-positive leukemia with either the CD28 or the 4-1BB costimulatory domain. In pediatric patients with relapsed/ refractory ALL, treatment with a CD28-CAR resulted in persistence which was limited to approximately 2 months in patients achieving remission.…”

Section: Anti G En P Os Itive E Sc Ape and C Ar T Cell Per S Is Ten Cementioning

confidence: 99%

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Immunobiology of chimeric antigen receptor T cells and novel designs

Walsh

Yang

Kohler

2019

Immunological Reviews

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Advances in the development of immunotherapies have offered exciting new options for the treatment of malignant diseases that are refractory to conventional cytotoxic chemotherapies. The adoptive transfer of T cells expressing chimeric antigen receptors (CARs) has demonstrated dramatic results in clinical trials and highlights the promise of novel immune‐based approaches to the treatment of cancer. As experience with CAR T cells has expanded with longer follow‐up and to a broader range of diseases, new obstacles have been identified which limit the potential lifelong benefits of CAR T cell therapy. These obstacles highlight not only the gaps in knowledge of the optimal clinical application of this “living drug”, but also gaps in our understanding of the fundamental biology of CAR T cells themselves. In this review, we discuss the obstacles facing CAR T cell therapy, how these relate to our current understanding of CAR T cell biology and approaches to enhance the clinical efficacy of this therapy.

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Section: Role Of Car Structure In Antigen Sensitivitymentioning

confidence: 83%

Section: Anti G En P Os Itive E Sc Ape and C Ar T Cell Per S Is Ten Cementioning

confidence: 99%

Immunobiology of chimeric antigen receptor T cells and novel designs

Walsh

Yang

Kohler

2019

Immunological Reviews

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“…T-cell isolation, lentivirus production and transduction, and ex vivo expansion of CAR T cells was performed as previously described 23 .…”

Section: Human T Cell Enrichment Lentivirus Production and Transductmentioning

confidence: 99%

“…Flow cytometric analysis was performed as previously described 23 . Tumor cells were identified using Ep-CAM (CD326) (BioLegend, Clone: 9C4).…”

Section: Intracellular/extracellular Staining and Flow Cytometrymentioning

confidence: 99%

Effective Combination Immunotherapy using Oncolytic Viruses to Deliver CAR Targets to Solid Tumors

Park

Fong

Chen

et al. 2019

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Chimeric antigen receptor (CAR)-engineered T cell therapy for solid tumors is limited by the lack of tumor-restricted and homogeneous expression of tumor antigens1,2. Therefore, we engineered an oncolytic virus to express a non-signaling, truncated CD19 (CD19t) protein for tumor-selective delivery, enabling targeting by CD19-specific CAR T cells. Infecting tumor cells with a chimeric oncolytic vaccinia virus coding for CD19t (OV19t) produced de novo CD19 surface-antigen expression prior to virus-mediated tumor lysis. Co-cultured CD19-CAR T cells secreted cytokines and elicited potent cytolytic activity against infected tumors. Using multiple mouse tumor models, intratumoral delivery of OV19t induced tumor expression of CD19t and improved tumor control following CD19-CAR T cell administration. CAR T cell–mediated tumor killing also promoted release of virus from dying tumor cells, which propogated tumor expression of CD19t. These data demonstrate a novel immunotherapy approach utilizing oncolytic viruses to promote de novo CAR T cell targeting of solid tumors.One Sentence SummaryWe describe a novel and effective combination immunotherapy utilizing oncolytic viruses to deliver de novo cell surface expression of CD19 antigen promoting CD19-CAR T cell anti-tumor responses against solid tumors.

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“…PBT030 endogenously expresses high level of IL13Ra2. HT1080 and PBT138 do not express IL13Ra2 and were lentivirally engineered to express varied levels based on different promoter strengths to investigate the relationship between killing kinetics and antigen expression level: High (>70% + ) driven by the EF1a promoter, Medium (between 40% + -70% + ) driven by the PGK promoter, Low (<20% + ) driven by the attenuated PGK100 promoter [35,36]. These cell lines are denoted with H, M, L respectively e.x.…”

Section: Cell Linesmentioning

confidence: 99%

Mathematical deconvolution of CAR T-cell proliferation and exhaustion from real-time killing assay data

Sahoo¹,

Yang²,

Abler³

et al. 2019

Preprint

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Chimeric antigen receptor (CAR) T-cell therapy has shown promise in the treatment of hematological cancers and is currently being investigated for solid tumors including high-grade glioma brain tumors. There is a desperate need to quantitatively study the factors that contribute to the efficacy of CAR T-cell therapy in solid tumors. In this work we use a mathematical model of predator-prey dynamics to explore the kinetics of CAR T-cell killing in glioma: the Chimeric Antigen Receptor t-cell treatment Response in GliOma (CARRGO) model. The model includes rates of cancer cell proliferation, CAR T-cell killing, CAR T-cell proliferation and exhaustion, and CAR T-cell persistence. We use patient-derived and engineered cancer cell lines with an in vitro real-time cell analyzer to parameterize the CARRGO model. We observe that CAR T-cell dose correlates inversely with the killing rate and correlates directly with the net rate of proliferation and exhaustion. This suggests that at a lower dose of CAR T-cells, individual T-cells kill more cancer cells but become more exhausted as compared to higher doses. Furthermore, the exhaustion rate was observed to increase significantly with tumor growth rate and was dependent on level of antigen expression. The CARRGO model highlights nonlinear dynamics involved in CAR T-cell therapy and provides novel insights into the kinetics of CAR T-cell killing. The model suggests that CAR T-cell treatment may be tailored to individual tumor characteristics including tumor growth rate and antigen level to maximize therapeutic benefit.Statement of SignificanceWe utilize a mathematical model to deconvolute the nonlinear contributions of CAR T-cell proliferation and exhaustion to predict therapeutic efficacy and dependence on CAR T-cell dose and target antigen levels.

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Co-stimulatory signaling determines tumor antigen sensitivity and persistence of CAR T cells targeting PSCA+ metastatic prostate cancer

Cited by 133 publications

References 45 publications

Immunobiology of chimeric antigen receptor T cells and novel designs

Immunobiology of chimeric antigen receptor T cells and novel designs

Effective Combination Immunotherapy using Oncolytic Viruses to Deliver CAR Targets to Solid Tumors

Mathematical deconvolution of CAR T-cell proliferation and exhaustion from real-time killing assay data

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