AI-Guided CAR Designs and AKT3 Degradation Synergize to Enhance Bispecific and Trispecific CAR-T Cell Persistence and Overcome Antigen Escape

  1. Mohammad Sufyan Ansari
  2. Varnit Chauhan
  3. Aashi Singh
  4. Areej Akhtar
  5. Nisha Chaudhary
  6. Reegina Tyagi
  7. Divya
  8. Kashif Husain
  9. Sheetal Sharma
  10. Ruquaiya Alam
  11. Md Shakir
  12. Mehak Pracha
  13. Samreen Anjum
  14. Mohd Nadeem
  15. Md Imam Faizan
  16. Iqbal Azmi
  17. Aditya Ramdas Iyer
  18. Pragya Gupta
  19. Mehwish Nafiz
  20. Shayan Ali
  21. Insha Mohi Uddin
  22. Momina Javid
  23. Hamenth Kumar P
  24. Amit Kumar Srivastava
  25. Ulaganathan Mabalirajan
  26. Vikram Mathews
  27. Sivaprakash Ramalingam
  28. Gaurav Kharya
  29. Tanveer Ahmad
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Abstract

The structural design of chimeric antigen receptors (CARs) is critical for achieving robust and durable anti-tumor responses, particularly when targeting multiple antigens to prevent tumor antigen escape. However, increasing CAR complexity can introduce structural vulnerabilities, leading to antigen-independent T cell activation, activation-induced cell death, and reduced CAR-T cell persistence. To overcome these challenges, we designed 10,824 CAR molecules across diverse formats and screened 1,452 constructs in-vitro to develop an artificial intelligence model, termed CAR-Mediated Self-Destruction (CARMSeD), which predicts CAR designs susceptible to self-activation and dysfunction. Guided by CARMSeD and structural CAR-CAR interaction modeling, we identified optimized CAR architectures incorporating ICOS and 4-1BB co-stimulatory domains. Humanized bispecific CARs targeting CD20/CD19 and CD22/CD19 demonstrated superior anti-tumor efficacy and persistence both in-vitro and in various xenograft mice models. To further extend CAR-T cell persistence, we engineered bispecific CARs integrated with an AKT3-targeted PROTAC strategy. Targeted degradation of AKT3 enhanced anti-tumor potency, promoted memory T cell formation, and enabled sustained responses even under tumor rechallenge and CD19 antigen-loss conditions. Mechanistically, these effects were mediated by metabolic reprogramming involving FOXO4; notably, FOXO4-deficient CAR-T cells exhibited impaired long-term persistence. Leveraging these mechanistic insights, we developed a trispecific CAR-T cell platform incorporating a bispecific T cell engager (BiTE) targeting CD22/CD3, combined with AKT3 PROTACs. These trispecific CAR-T cells achieved potent tumor eradication, even against malignancies lacking both CD19 and CD20 expression. Collectively, this study presents a comprehensive strategy combining structure-based design, AI-guided screening, and targeted protein degradation to engineer next-generation bi and trispecific CAR-T cells with enhanced persistence, broad antigen coverage, and superior therapeutic durability.

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  1. Version published to 10.1101/2025.06.12.658477v3 on bioRxiv
  2. Version published to 10.1101/2025.06.12.658477v1 on bioRxiv
  3. Version published to 10.1101/2025.06.12.658477v2 on bioRxiv