CAR Intrinsic Design Pre-Shapes Transcriptional and Metabolic Networks in CAR T Cells
Didem Agac Cobanoglu, Samantha Franklin, Yue Hu, Devon J. Boland, Xiaotong Song

TL;DR
This study shows how CAR design and metabolic support influence the baseline activity of CAR T cells, even without cancer cell contact.
Contribution
The study reveals that CAR design and metabolic refueling pre-program CAR T cells through tonic NF-κB activation and transcriptional changes.
Findings
CAR T cells show baseline NF-κB-driven inflammatory activation regardless of antigen exposure.
Metabolic refueling enhances inflammatory and survival programs in CAR T cells without changing their direction.
GPC3 CAR T cells exhibit stronger baseline activation than HER2 CAR T cells.
Abstract
Background/Objectives: Chimeric antigen receptor (CAR) T cells are a powerful cancer therapy, but their function depends heavily on internal signaling domains and metabolic adaptability. Most studies evaluate CAR behavior upon antigen exposure, yet intrinsic signaling properties may pre-program CAR T cell states even in the absence of stimulation. This study investigates how CAR design and metabolic support shape baseline transcriptional programs, focusing on tonic signaling and NF-κB-related pathways. Methods: We engineered CAR T cells targeting HER2 or GPC3 antigens, incorporating either 4-1BB or CD28 co-stimulatory domains, respectively. A subset of cells was further modified with adenosine deaminase 1 (ADA1) and CD26 to degrade extracellular adenosine and supply inosine, a metabolic strategy termed metabolic refueling (MR). Bulk RNA-seq was performed on resting T cells without…
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Taxonomy
TopicsCAR-T cell therapy research · Immune Cell Function and Interaction · Viral Infectious Diseases and Gene Expression in Insects
