AI Article Synopsis

  • Base editing is a new gene-editing technique that allows targeted genetic changes without harmful DNA breaks, using enzymes usually delivered as costly linear mRNA.
  • Researchers have developed a more affordable method using circular RNA (circRNA), which shows higher editing efficiency and reduces RNA requirements by eight times.
  • This approach successfully produced a clinical dose of CAR T cells with up to 86% editing efficiency, highlighting circRNA's potential to lower costs and improve large-scale production of genetically modified cells.

Article Abstract

Base editing is a revolutionary gene-editing technique enabling the introduction of point mutations into the genome without generating detrimental DNA double-stranded breaks. Base-editing enzymes are commonly delivered in the form of modified linear messenger RNA (mRNA) that is costly to produce. Here, we address this problem by developing a simple protocol for manufacturing base-edited cells using circular RNA (circRNA), which is less expensive to synthesize. Compared with linear mRNA, higher editing efficiencies were achieved with circRNA, enabling an 8-fold reduction in the amount of RNA required. We used this protocol to manufacture a clinical dose (1 × 10 cells) of base-edited chimeric antigen receptor (CAR) T cells lacking expression of the inhibitory receptor, PD-1. Editing efficiencies of up to 86% were obtained using 0.25 μg circRNA/1 × 10 cells. Increased editing efficiencies with circRNA were attributed to more efficient translation. These results suggest that circRNA, which is less expensive to produce than linear mRNA, is a viable option for reducing the cost of manufacturing base-edited cells at scale.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10597784PMC
http://dx.doi.org/10.1016/j.omtm.2023.101123DOI Listing

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