Chimeric Antigen Receptor T-cell Therapy in Cancer: A Critical Review

Ravikant Sharma; Lalitha Suravarjhula; Madhuparna Banerjee; Gautam Kumar; Nitesh Kumar

doi:10.2174/2589977515666230220092125

Chimeric Antigen Receptor T-cell Therapy in Cancer: A Critical Review

Curr Drug Res Rev. 2023;15(3):241-261. doi: 10.2174/2589977515666230220092125.

Authors

Ravikant Sharma^{1

2}, Lalitha Suravarjhula³, Madhuparna Banerjee³, Gautam Kumar³, Nitesh Kumar⁴

Affiliations

¹ Department of Biotechnology, National Institution of Pharmaceutical Education and Research, Hajipur, Vaishali, 844102, Bihar, India.
² Research Institute of Biomedicine, University of Oulu, Aapistie 5, Oulu, 90014, Finland.
³ Department of Pharmacology, Manipal College of Pharmaceutical Sciences, Manipal Academy of Higher Education, Manipal, Karnataka, 576104, India.
⁴ Department of Pharmacology and Toxicology, National Institution of Pharmaceutical Education and Research, Hajipur, Vaishali, Bihar, 844102, India.

PMID: 36825696
DOI: 10.2174/2589977515666230220092125

Abstract

Targeted cancer therapy acts on targeted molecules, is less toxic to normal cells, and acts more specifically on cancer cells. The two primary strategies for preventing malignancy growth are the blocking of T-cell repression signals or forwarding of T-cell to tumor target with both T and tumor-specific antibodies. The CAR comprises three domains, the extracellular antigen recognition domain and the intracellular T-cell signaling domain, which participate in activating T-cells. The two most common adverse effects of CAR T-cell treatment are cytokine release syndrome (CRS) and cell-associated neurotoxicity syndrome (CANS). The adaptability of intracellular signaling domains inside CARs allows the cell to counterbalance the downregulation of costimulatory molecules produced by tumor cells, either indirectly or directly. The major disadvantage of CAR-T cell therapy is off-target toxicity. Treatment with CARs expressing CD3, CD123, Lewis Y, CLL-1, CD44v6, FLT3, and folate receptors showed promising results in preclinical models of acute myeloid leukemia (AML). A recent study has revealed that B7-H3 CART cells exhibit significant anticancer efficacy in a variety of solid tumor preclinical models, including PDAC, ovarian cancer, neuroblastoma, and various pediatric malignancies. The notion of SUPRA CAR, with its unique capacity to alter targets without the need to re-engineer, is a recent innovation in CAR. Given the importance of NK cells in tumor development and metastatic defence, NK cell-based immunotherapies, including adoptive transfer of NK cells, have garnered a lot of interest. With the advancement of improved cellular manufacturing methods, novel cellular engineering strategies, precision genome editing technologies, and combination therapy approaches, we firmly believe that CAR-T cells will soon become an off-the-shelf, cost-effective, and potentially curative therapy for oncogenesis.

Keywords: CAR-T Cell; CD19; CD28; CD3; bispecific T-cell products; cancer.

Publication types

Review

MeSH terms

Cell Line, Tumor
Cell- and Tissue-Based Therapy
Child
Cytotoxicity, Immunologic
Humans
Leukemia, Myeloid, Acute* / pathology
Leukemia, Myeloid, Acute* / therapy
Receptors, Chimeric Antigen* / genetics

Substances

Receptors, Chimeric Antigen
cell-associated neurotoxicity