Choice of costimulatory domains and of cytokines determines CAR T-cell activity in neuroblastoma

Quintarelli, Concetta; Orlando, Domenico; Boffa, Iolanda; Guercio, Marika; Polito, Vinicia Assunta; Petretto, Andrea; Lavarello, Chiara; Sinibaldi, Matilde; Weber, Gerrit; Bufalo, Francesca Del; Giorda, Ezio; Scarsella, Marco; Petrini, Stefania; Pagliara, Daria; Locatelli, Franco; Angelis, Biagio De; Caruana, Ignazio

doi:10.1080/2162402x.2018.1433518

Cited by 112 publications

(92 citation statements)

References 61 publications

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“…However, preclinical models and exploratory comparisons between single-arm clinical studies suggest CAR T cells incorporating each of these domains may differ qualitatively. 11,24,25,29,50,56,68 In animal studies, CD28-costimulated CAR T cells exhibit improved early expansion and cytotoxic activity compared to their 41BB-costimulated counterparts in vivo, while 41BB-costimulated CAR T cells exhibit better long-term persistence. 27 Consistent with this, pharmacokinetic analyses of phase 2 CAR T cell clinical trials in r/r B-NHL suggest that CD28-containing second-generation anti-CD19 CAR T cells peak earlier but persist less well than 41BB-incorporating CAR T cells.…”

Section: Disease-specific Indications For Use Of Costimulatory Domainsmentioning

confidence: 99%

Selecting costimulatory domains for chimeric antigen receptors: functional and clinical considerations

et al. 2019

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Costimulatory signals are required to achieve robust chimeric antigen receptor (CAR) T cell expansion, function, persistence and antitumor activity. These can be provided by incorporating intracellular signalling domains from one or more T cell costimulatory molecules, such as CD28 or 4‐1BB, into the CAR. The selection and positioning of costimulatory domains within a CAR construct influence CAR T cell function and fate, and clinical experience of autologous anti‐CD19 CAR T cell therapies suggests that costimulatory domains have differential impacts on CAR T cell kinetics, cytotoxic function and potentially safety profile. The clinical impacts of combining costimulatory domains and of alternative costimulatory domains are not yet clearly established, and may be construct‐ and disease‐specific. The aim of this review is to summarise the function and effect of established and emerging costimulatory domains and their combinations within CAR T cells.

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Section: Disease-specific Indications For Use Of Costimulatory Domainsmentioning

confidence: 99%

Selecting costimulatory domains for chimeric antigen receptors: functional and clinical considerations

et al. 2019

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“…However, to compare the outcome using two different antibodies, recognizing different epitopes, might not have a clear scientific value. One would need to put FRP5 scFv on a third‐generation construct or trastuzumab on the second generation to be able to conclude on the main cause of this discrepancy, as recently depicted with GD2 CAR . One potential strategy for improving cancer specificity and clinical response is to target not only one, but two tumour‐associated antigens on a single cancer cell by a bispecific CAR T‐cell molecule .…”

Section: Human Epidermal Growth Factor Receptor 2 (Her2)mentioning

confidence: 99%

Treating osteosarcoma with CAR T cells

et al. 2019

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Novel therapies to treat patients with solid cancers that have developed resistance to chemotherapy represent unmet needs of considerable dimensions. In the present review, we will address the attempts to develop chimeric antigen receptor (CAR) targeted immunotherapy against osteosarcoma (OS). This aggressive cancer displays its peak incidence in children and young adults. The main cause of patient death is lung metastases with a 5-year survival as low as 5%-10% in the primary metastatic setting and 30% in the relapse situation, respectively. Effective adjuvant combination chemotherapy introduced more than 40 years ago improved the survival rates from below 20% to around 60% in patients; however, since then, no major breakthroughs have been made. The use of immune checkpoint inhibitors has been disappointing in OS, while other types of immunotherapies such as CAR T cells remain largely unexplored. Indeed, for CAR T-cell therapy to be efficacious, two main criteria need to be fulfilled: (a) CAR T cells should target an epitope selectively expressed on the cell surface of OS in order to prevent toxicities in normal tissues and (b) the target should also be widely expressed on OS metastases. These challenges have already been undertaken in OS and illustrate the difficulties in developing tomorrow's CAR-T treatment in a solid tumour. We will discuss the experiences with CAR-T therapy development and efficacy to combat the clinical challenges in OS.

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“…Combination therapy using a-PD-1 demonstrated superior antitumor efficacy in an in vivo model compared to conventional CAR T cells that correlated with enhanced effector function of the CAR T cells such as granzyme B and IFNc upon PD-1 blockade. 16,17 In the context of costimulation using exogenous antibodies, a recent preclinical study tested the combination of Her2-specific CAR T cells with a-4-1BB therapy against Her2-expressing solid tumors. 12 The clinical translation of CAR T-cell and a-PD-1 mAb is now underway with multiple clinical trials currently recruiting patients.…”

Section: Using Immunomodulatory Antibodies To Enhance Car T-cell Antimentioning

confidence: 99%

“…16 Both 4-1BB-and/or OX40-containing CAR T cells have been tested in various preclinical studies; however, comparisons between the two domains remain inconclusive in terms of overall antitumor effect observed given variability in the models used from different groups. 16,17 In the context of costimulation using exogenous antibodies, a recent preclinical study tested the combination of Her2-specific CAR T cells with a-4-1BB therapy against Her2-expressing solid tumors. The combination treatment resulted in significantly enhanced tumor regression compared to CAR T-cell therapy alone or control T cells in combination with a-4-1BB mAb.…”

Section: Using Immunomodulatory Antibodies To Enhance Car T-cell Antimentioning

confidence: 99%

Switching on the green light for chimeric antigen receptor T‐cell therapy

et al. 2019

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Adoptive cellular therapy involving genetic modification of T cells with chimeric antigen receptor (CAR) transgene offers a promising strategy to broaden the efficacy of this approach for the effective treatment of cancer. Although remarkable antitumor responses have been observed following CAR T‐cell therapy in a subset of B‐cell malignancies, this has yet to be extended in the context of solid cancers. A number of promising strategies involving reprogramming the tumor microenvironment, increasing the specificity and safety of gene‐modified T cells and harnessing the endogenous immune response have been tested in preclinical models that may have a significant impact in patients with solid cancers. This review will discuss these exciting new developments and the challenges that must be overcome to deliver a more sustained and potent therapeutic response.

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Choice of costimulatory domains and of cytokines determines CAR T-cell activity in neuroblastoma

Cited by 112 publications

References 61 publications

Selecting costimulatory domains for chimeric antigen receptors: functional and clinical considerations

Selecting costimulatory domains for chimeric antigen receptors: functional and clinical considerations

Treating osteosarcoma with CAR T cells

Switching on the green light for chimeric antigen receptor T‐cell therapy

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