Frontiers in Immunology (Nov 2023)

Humanized single-domain antibody targeting HER2 enhances function of chimeric antigen receptor T cells

  • Rui Zheng,
  • Yuankun Chen,
  • Yiting Zhang,
  • Sixin Liang,
  • Sixin Liang,
  • Xiaojuan Zhao,
  • Yiyi Wang,
  • Yiyi Wang,
  • Pengju Wang,
  • Pengju Wang,
  • Ruotong Meng,
  • Ruotong Meng,
  • Angang Yang,
  • Bo Yan

DOI
https://doi.org/10.3389/fimmu.2023.1258156
Journal volume & issue
Vol. 14

Abstract

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IntroductionChimeric antigen receptors (CARs) can redirect T cells against antigen-expressing tumors, and each component plays an important role in the function and anti-tumor efficacy. It has been reported that using human sequences or a low affinity of CAR single-chain variable fragments (scFvs) in the CAR binding domains is a potential way to enhance the function of CAR-T cells. However, it remains largely unknown how a lower affinity of CARs using humanized scFvs affects the function of CAR-T cells until recently.MethodsWe used different humanized anti-HER2 antibodies as the extracellular domain of CARs and further constructed a series of the CAR-T cells with different affinity.ResultsWe have observed that moderately reducing the affinity of CARs (light chain variable domain (VL)-based CAR-T) could maintain the anti-tumor efficacy, and improved the safety of CAR therapy both in vitro and in vivo compared with high-affinity CAR-T cells. Moreover, T cells expressing the VL domain only antibody exhibited long-lasting tumor elimination capability after multiple challenges in vitro, longer persistence and lower cytokine levels in vivo.DiscussionOur findings provide an alternative option for CAR-T optimization with the potential to widen the use of CAR T cells.

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