Intracavitary ‘T4 immunotherapy’ of malignant mesothelioma using pan-ErbB re-targeted CAR T-cells

Klampatsa, Astero; Achkova, Daniela; Davies, Daniel; Parente-Pereira, Ana C.; Woodman, Natalie; Rosekilly, James; Osborne, Georgina F; Thayaparan, Thivyan; Billè, Andrea; Sheaf, Michael; Spicer, James; King, Juliet; Maher, John

doi:10.1016/j.canlet.2017.02.015

Cited by 52 publications

(45 citation statements)

References 43 publications

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“…Analysis of a larger series of MPM that contained the subset presented here confirmed, as expected, that epithelioid tumors were associated with improved patient survival. 15 Expression of MET was detected by immunohistochemistry in 67.6% of MPM, either at low (28.1%), intermediate (24.6%) or high intensity (14.9%). Receptor distribution was cytoplasmic with membranous accentuation (Fig.…”

Section: Expression Of Met By Malignant Pleural Mesotheliomasmentioning

confidence: 94%

“…14 In keeping with this, we have recently demonstrated that ErbB re-targeted CAR T-cells achieve significant antitumor activity combined with excellent safety in pre-clinical models of malignant pleural mesothelioma (MPM). 15 The MET receptor tyrosine kinase is also aberrantly expressed in a large proportion of mesotheliomas [16][17][18][19][20][21] and has been proposed as an attractive therapeutic target in this disease. 18,22,23 Disappointingly however, a phase II trial of the selective MET inhibitor tivantinib has recently been terminated (https://clini caltrials.gov/ct2/show/NCT01861301; accessed March 25th, 2017).…”

Section: Introductionmentioning

confidence: 99%

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CAR T-cell immunotherapy of MET-expressing malignant mesothelioma

et al. 2017

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Mesothelioma is an incurable cancer for which effective therapies are required. Aberrant MET expression is prevalent in mesothelioma, although targeting using small molecule-based therapeutics has proven disappointing. Chimeric antigen receptors (CARs) couple the HLA-independent binding of a cell surface target to the delivery of a tailored T-cell activating signal. Here, we evaluated the anti-tumor activity of MET re-targeted CAR T-cells against mesothelioma. Using immunohistochemistry, MET was detected in 67% of malignant pleural mesotheliomas, most frequently of epithelioid or biphasic subtype. The presence of MET did not influence patient survival. Candidate MET-specific CARs were engineered in which a CD28+CD3ζ endodomain was fused to one of 3 peptides derived from the N and K1 domains of hepatocyte growth factor (HGF), which represents the minimum MET binding element present in this growth factor. Using an NIH3T3-based artificial antigen-presenting cell system, we found that all 3 candidate CARs demonstrated high specificity for MET. By contrast, these CARs did not mediate T-cell activation upon engagement of other HGF binding partners, namely CD44v6 or heparan sulfate proteoglycans, including Syndecan-1. NK1-targeted CARs demonstrated broadly similar potency, indicated by destruction of MET-expressing mesothelioma cell lines, accompanied by cytokine release. anti-tumor activity was demonstrated following intraperitoneal delivery to mice with an established mesothelioma xenograft. Progressive tumor regression occurred without weight loss or other clinical indicators of toxicity. These data confirm the frequent expression of MET in malignant pleural mesothelioma and demonstrate that this can be targeted effectively and safely using a CAR T-cell immunotherapeutic strategy.

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Section: Expression Of Met By Malignant Pleural Mesotheliomasmentioning

confidence: 94%

Section: Introductionmentioning

confidence: 99%

CAR T-cell immunotherapy of MET-expressing malignant mesothelioma

et al. 2017

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“…These products are Major Histocompatibility Complex (MHC)-independent, meaning they can be utilised in diverse populations. Anti-mesothelin and anti-fibroblast activation protein (FAP; which is expressed ubiquitously in the MPM tumour microenvironment) CAR T-lymphocytes have both been shown to induce regression in MPM xenograft tumour models and can be delivered locally, to the pleura, using an indwelling pleural catheter [78,79]. Several Phase I studies testing the safety of these approaches are currently underway.…”

Section: Immunotherapymentioning

confidence: 99%

Progress and challenges in Mesothelioma: From bench to bedside

Blyth

Murphy

2018

Respiratory Medicine

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Malignant Pleural Mesothelioma (MPM) is currently an incurable cancer with a typical survival of 1 year from the time of diagnosis. The recent genomic and transcriptomic characterization of MPM presents new opportunities and challenges for MPM researchers. Recent advances in clinical and laboratory diagnostics, and proposals for an updated, data-driven, staging system, also present new challenges for clinicians and hospital services involved in MPM care. The aim of this review is first to introduce the reader to the topic of MPM, a disease that is causally linked to prior, typically occupational, exposure to asbestos fibres. Secondly, we will discuss MPM from the clinical and laboratory perspectives, including reviews of current and evolving therapies and our present understanding of the molecular basis of the disease. Finally, we will attempt to identify critical knowledge gaps that currently prevent more effective treatment, including the challenges involved in early detection and chemoprophylaxis.

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“…Amongst the CARs brought into the clinic (Table 1), the ligand-based CARs IL-13Rα and T1E are the ones with clinical information available [36, 46, 57–59]. …”

Section: Natural Receptor- and Ligand-based Cars Tested In The Clinicmentioning

confidence: 99%

Advances in the use of natural receptor- or ligand-based chimeric antigen receptors (CARs) in haematologic malignancies

Murad

Graber

Sentman

2018

Best Practice & Research Clinical Haematology

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Chimeric antigen receptors (CAR)-T cell therapy has recently made promising advances towards treatment of B-cell malignancies. This approach makes use of an antibody-derived single chain variable fragment (scFv)-based CAR to target the CD19 antigen. Currently scFvs are the most common strategy for creation of CARs, but tumor cells can also be targeted using non-antibody based approaches with designs focused on the interaction between natural receptors and their ligands. This emerging strategy has been used in unique ways to target multiple tumor types, including solid and haematological malignancies. In this review, we will highlight the performance of receptor-ligand combinations as designs for CARs to treat cancer, with a particular focus on haematologic malignancies.

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Intracavitary ‘T4 immunotherapy’ of malignant mesothelioma using pan-ErbB re-targeted CAR T-cells

Cited by 52 publications

References 43 publications

CAR T-cell immunotherapy of MET-expressing malignant mesothelioma

CAR T-cell immunotherapy of MET-expressing malignant mesothelioma

Progress and challenges in Mesothelioma: From bench to bedside

Advances in the use of natural receptor- or ligand-based chimeric antigen receptors (CARs) in haematologic malignancies

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