Immuno-Oncology and Technology (Jun 2023)

Non-viral chimeric antigen receptor (CAR) T cells going viral

  • H. Balke-Want,
  • V. Keerthi,
  • A. Cadinanos-Garai,
  • C. Fowler,
  • N. Gkitsas,
  • A.K. Brown,
  • R. Tunuguntla,
  • M. Abou-el-Enein,
  • S.A. Feldman

Journal volume & issue
Vol. 18
p. 100375

Abstract

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Chimeric antigen receptor (CAR) T cell therapy has made significant strides in the treatment of B-cell malignancies, but its application in treating solid tumors still poses significant challenges. Particularly, the widespread use of viral vectors to deliver CAR transgenes into T cells comes with limitations, including high costs and regulatory restrictions, which hinder the translation of novel genetic engineering concepts into clinical applications. Non-viral methods, such as transposon/transposase and clustered regularly interspaced short palindromic repeats (CRISPR)/Cas systems, offer promising alternatives for stable transgene insertion in CAR-T cells. These methods offer the potential to increase accessibility and efficiency in the development and delivery of CAR-T cell therapies. The main challenge in using non-viral methods, however, is their low knock-in efficiency, which leads to low transgene expression levels. In this review, we discuss recent developments in non-viral approaches for CAR-T cell production, the manufacturing requirements for clinical-grade production of non-viral CAR-T cells, and the adjustments needed in quality control for proper characterization of genomic features and evaluation of potential genotoxicity.

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