Intrinsic ADRB2 inhibition improves CAR-T cell therapy efficacy against prostate cancer

  • Iqra Ajmal
  • , Muhammad Asad Farooq
  • , Yixin Duan
  • , Jie Yao
  • , Yaoxin Gao
  • , Xinhui Hui
  • , Yujia Ge
  • , Yiran Chen
  • , Yaojun Ren
  • , Bingtan Du
  • , Wenzheng Jiang*
  • *Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

15 Scopus citations

Abstract

Chimeric antigen receptor (CAR)-T cell therapy has shown limited success in patients with solid tumors. Recent in vitro and in vivo data have shown that adrenoceptor beta-2 (ADRB2) is a novel checkpoint receptor that inhibits T cell-mediated anti-tumor responses. To inhibit ADRB2-mediated inhibitory signaling, we downregulated ADRB2 in CAR-T (shβ2-CAR-T) cells via RNA interference, assessed different parameters, and compared them with conventional second-generation CAR-T cells. ADRB2 knockdown CAR-T cells exhibited enhanced cytotoxicity against prostate cancer cell lines in vitro, by increasing CD69, CD107a, GzmB, IFN-γ, T-bet, and GLUT-1. In addition, ADRB2 deficiency led to improved proliferation, increased CD8/CD4 T cell ratio, and decreased apoptosis in CAR-T cells. shβ2-CAR-T cells expressed more Bcl-2 and led to the generation of more significant proportions of T central memory cells. Finally, the ZAP-70/NF-κB signaling axis was shown to be responsible for the improved functions of novel CAR-T cells. In tumor-bearing mice, shβ2-CAR-T cells performed better than conventional CAR-T cells in eradicating prostate tumors. The study provides the basis for future clinical and translational CAR-T cell research to focus on adrenergic stress-mediated challenges in the tumor microenvironment of stressed tumors.

Original languageEnglish
Pages (from-to)3539-3557
Number of pages19
JournalMolecular Therapy
Volume32
Issue number10
DOIs
StatePublished - 2 Oct 2024

Keywords

  • ADRB2
  • CAR
  • CAR-T cell therapy
  • adrenergic stress
  • adrenoceptor beta-2
  • chimeric antigen receptor
  • combination therapy
  • immune checkpoint
  • immunotherapy
  • neuroimmunology
  • prostate cancer
  • tumor microenvironment

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