Immunotherapy of malignant disease using chimeric antigen receptor engrafted T cells

John Maher¹

Affiliations

Affiliation

¹ CAR Mechanics Group, Department of Research Oncology, King's Health Partners Integrated Cancer Centre, King's College London, Guy's Hospital Campus, Great Maze Pond, London SE1 9RT, UK ; Department of Immunology, Barnet and Chase Farm Hospitals NHS Trust, Barnet, Hertfordshire EN5 3DJ, UK ; Department of Clinical Immunology and Allergy, King's College Hospital NHS Foundation Trust, Denmark Hill, London SE5 9RS, UK.

PMID: 23304553
PMCID: PMC3523553
DOI: 10.5402/2012/278093

Immunotherapy of malignant disease using chimeric antigen receptor engrafted T cells

John Maher. ISRN Oncol. 2012.

. 2012:2012:278093.

doi: 10.5402/2012/278093. Epub 2012 Dec 9.

Author

John Maher¹

Affiliation

¹ CAR Mechanics Group, Department of Research Oncology, King's Health Partners Integrated Cancer Centre, King's College London, Guy's Hospital Campus, Great Maze Pond, London SE1 9RT, UK ; Department of Immunology, Barnet and Chase Farm Hospitals NHS Trust, Barnet, Hertfordshire EN5 3DJ, UK ; Department of Clinical Immunology and Allergy, King's College Hospital NHS Foundation Trust, Denmark Hill, London SE5 9RS, UK.

PMID: 23304553
PMCID: PMC3523553
DOI: 10.5402/2012/278093

Abstract

Chimeric antigen receptor- (CAR-) based immunotherapy has been under development for almost 25 years, over which period it has progressed from a new but cumbersome technology to an emerging therapeutic modality for malignant disease. The approach involves the genetic engineering of fusion receptors (CARs) that couple the HLA-independent binding of cell surface target molecules to the delivery of a tailored activating signal to host immune cells. Engineered CARs are delivered most commonly to peripheral blood T cells using a range of vector systems, most commonly integrating viral vectors. Preclinical refinement of this approach has proceeded over several years to the point that clinical testing is now being undertaken at several centres, using increasingly sophisticated and therapeutically successful genetic payloads. This paper considers several aspects of the pre-clinical and clinical development of CAR-based immunotherapy and how this technology is acquiring an increasing niche in the treatment of both solid and haematological malignancies.

PubMed Disclaimer

Figures

**Figure 1**
Generic structure of a chimeric antigen receptor (CAR). These fusion receptors comprise a targeting moiety (in this example, an antibody-derived single chain antibody (scFv)), coupled via a hinge and transmembrane element to a bespoke modular signalling domain. This example shows a “third generation” CAR in which signalling is provided by CD3ζ together with costimulation provided by CD28 and a tumour necrosis factor receptor (TNFr), such as 4-1BB or OX40.

See this image and copyright information in PMC

Cited by

Development of third generation anti-EGFRvIII chimeric T cells and EGFRvIII-expressing artificial antigen presenting cells for adoptive cell therapy for glioma.
Sahin A, Sanchez C, Bullain S, Waterman P, Weissleder R, Carter BS. Sahin A, et al. PLoS One. 2018 Jul 5;13(7):e0199414. doi: 10.1371/journal.pone.0199414. eCollection 2018. PLoS One. 2018. PMID: 29975720 Free PMC article.
Oncolytic Virus Combination Therapy: Killing One Bird with Two Stones.
Martin NT, Bell JC. Martin NT, et al. Mol Ther. 2018 Jun 6;26(6):1414-1422. doi: 10.1016/j.ymthe.2018.04.001. Epub 2018 Apr 5. Mol Ther. 2018. PMID: 29703699 Free PMC article. Review.
Combining Cell and Gene Therapy in an Effort to Eradicate HIV.
Wagner TA. Wagner TA. AIDS Patient Care STDS. 2016 Dec;30(12):534-538. doi: 10.1089/apc.2016.0226. AIDS Patient Care STDS. 2016. PMID: 27905840 Free PMC article.
Genetically modified T cells in cancer therapy: opportunities and challenges.
Sharpe M, Mount N. Sharpe M, et al. Dis Model Mech. 2015 Apr;8(4):337-50. doi: 10.1242/dmm.018036. Epub 2015 Apr 1. Dis Model Mech. 2015. PMID: 26035842 Free PMC article. Review.
Immunotherapy with CAR-Modified T Cells: Toxicities and Overcoming Strategies.
Sun S, Hao H, Yang G, Zhang Y, Fu Y. Sun S, et al. J Immunol Res. 2018 Apr 17;2018:2386187. doi: 10.1155/2018/2386187. eCollection 2018. J Immunol Res. 2018. PMID: 29850622 Free PMC article. Review.

See all "Cited by" articles

References

1. Töpfer K, Kempe S, Müller N, et al. Tumor evasion from T cell surveillance. Journal of Biomedicine and Biotechnology. 2011;2011918471 - PMC - PubMed
1. Landsberg J, Kohlmeyer J, Renn M, et al. Melanomas resist T-cell therapy through inflammation-induced reversible dedifferentiation. Nature. 2012;490(7420):412–416. - PubMed
1. Rosenberg SA, Yang JC, Restifo NP. Cancer immunotherapy: moving beyond current vaccines. Nature Medicine. 2004;10(9):909–915. - PMC - PubMed
1. Willemsen RA, Ronteltap C, Chames P, Debets R, Bolhuis RLH. T cell retargeting with MHC class I-restricted antibodies: the CD28 costimulatory domain enhances antigen-specific cytotoxicity and cytokine production. Journal of Immunology. 2005;174(12):7853–7858. - PubMed
1. Stewart-Jones G, Wadle A, Hombach A, et al. Rational development of high-affinity T-cell receptor-like antibodies. Proceedings of the National Academy of Sciences of the United States of America. 2009;106(14):5784–5788. - PMC - PubMed

LinkOut - more resources

Full Text Sources
Other Literature Sources
- The Lens - Patent Citations Database
Research Materials
- NCI CPTC Antibody Characterization Program

Save citation to file

Email citation

Add to Collections

Add to My Bibliography

Your saved search

Create a file for external citation management software

Your RSS Feed

Immunotherapy of malignant disease using chimeric antigen receptor engrafted T cells

Affiliation

Immunotherapy of malignant disease using chimeric antigen receptor engrafted T cells

Author

Affiliation

Abstract

Figures

Similar articles

Cited by

References

LinkOut - more resources

Full Text Sources

Other Literature Sources

Research Materials