Skip to main page content
U.S. flag

An official website of the United States government

Dot gov

The .gov means it’s official.
Federal government websites often end in .gov or .mil. Before sharing sensitive information, make sure you’re on a federal government site.

Https

The site is secure.
The https:// ensures that you are connecting to the official website and that any information you provide is encrypted and transmitted securely.

Access keys NCBI Homepage MyNCBI Homepage Main Content Main Navigation
Review
. 2019 May 20;8(5):e1050.
doi: 10.1002/cti2.1050. eCollection 2019.

Clinical chimeric antigen receptor-T cell therapy: a new and promising treatment modality for glioblastoma

Michael P Brown  1   2   3 Lisa M Ebert  1 Tessa Gargett  1
Affiliations
Review

Clinical chimeric antigen receptor-T cell therapy: a new and promising treatment modality for glioblastoma

Michael P Brown et al. Clin Transl Immunology. .

Erratum in

Abstract

Chimeric antigen receptor (CAR)-T cell therapy is now approved in the United States and Europe as a standard treatment for relapsed/refractory B-cell malignancies. It has also been approved recently by the Therapeutic Goods Administration in Australia and may soon be publicly reimbursed. This advance has accentuated scientific, clinical and commercial interest in adapting this exciting technology for the treatment of solid cancers where it is widely recognised that the challenges of overcoming a hostile tumor microenvironment are most acute. Indeed, CAR-T cell technology may be of the greatest value for those cancers that lack pre-existing immunity because they are immunologically 'cold', or have a low somatic tumor mutation load, or both. These cancers are generally not amenable to therapeutic immune checkpoint blockade, but CAR-T cell therapy may be effective because it provides an abundant supply of autologous tumor-specific T cells. This is achieved by using genetic engineering to re-direct autologous T-cell cytotoxicity towards a tumor-associated antigen, bypassing endogenous T-cell requirements for antigen processing, MHC-dependent antigen presentation and co-stimulation. One of the most challenging solid cancers is glioblastoma, which has among the least permissive immunological milieu of any cancer, and which is almost always fatal. Here, we argue that CAR-T cell technology may counter some glioblastoma defences and provide a beachhead for furthering our eventual therapeutic aims of restoring effective antitumor immunity. Although clinical investigation of CAR-T cell therapy for glioblastoma is at an early stage, we discuss three recently published studies, which feature significant differences in target antigen, CAR-T cell phenotype, route of administration and tumor response. We discuss the lessons, which may be learned from these studies and which may guide further progress in the field.

Keywords: T cells; chimeric antigen receptor; glioblastoma; neurotoxicity.

PubMed Disclaimer

Conflict of interest statement

The authors declare no conflict of interest.

References

    1. Lim M, Xia Y, Bettegowda C, Weller M. Current state of immunotherapy for glioblastoma. Nat Rev Clin Oncol 2018; 15: 422–442. - PubMed
    1. Hodges TR, Ott M, Xiu J, et al Mutational burden, immune checkpoint expression, and mismatch repair in glioma: implications for immune checkpoint immunotherapy. Neuro Oncol 2017; 19: 1047–1057. - PMC - PubMed
    1. Sadelain M, Riviere I, Riddell S. Therapeutic T cell engineering. Nature 2017; 545: 423–431. - PMC - PubMed
    1. Australian Institute of Health and Welfare . Brain and other central nervous system cancers. 2017; Cat. no. CAN 106. Canberra: AIHW.
    1. Hanif F, Muzaffar K, Perveen K, Malhi SM, Simjee S. Glioblastoma multiforme: a review of its epidemiology and pathogenesis through clinical presentation and treatment. Asian Pac J Cancer Prev 2017; 18: 3–9. - PMC - PubMed

LinkOut - more resources