Background The field of synthetic biology aims to engineer living organisms for specific therapeutic applications, with CAR-T cell therapy emerging as a groundbreaking approach in cancer treatment due to its potential for flexibility, specificity, predictability, and controllability. CAR-T cell therapies involve the genetic modification of T cells to target tumor-specific antigens. However, challenges persist because the limited spatio-temporal resolution in current models hinders the therapy’s safety, cost-effectiveness, and overall potential, particularly for solid tumors Main body This manuscript explores how mathematical models and computational techniques can enhance CAR-T therapy design and predict therapeutic outcomes, focusing on critical factors such as antigen receptor functionality, treatment efficacy, and potential adverse effects. We examine CAR-T cell dynamics and the impact of antigen binding, addressing strategies to overcome antigen escape, cytokine release syndrome, and relapse. Conclusion We propose a comprehensive framework for using these models to advance CAR-T cell therapy, bridging the gap between existing therapeutic methods and the full potential of CAR-T engineering and its clinical application.
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Guido Putignano
Samuel Ruipérez-Campillo
Zhou Yuan
Frontiers in Immunology
University of Southern California
ETH Zurich
Universidad de Granada
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Putignano et al. (Fri,) studied this question.
www.synapsesocial.com/papers/68c1a5ff54b1d3bfb60e012f — DOI: https://doi.org/10.3389/fimmu.2025.1581210