Scientific Reports (Mar 2022)

Humanization of a strategic CD3 epitope enables evaluation of clinical T-cell engagers in a fully immunocompetent in vivo model

  • Julie A. Zorn,
  • Matthew L. Wheeler,
  • Ralston M. Barnes,
  • Jim Kaberna,
  • Winse Morishige,
  • Marek Harris,
  • Richard Y.-C. Huang,
  • Jack Lohre,
  • Yu Ching Chang,
  • Bryant Chau,
  • Kathleen Powers,
  • Ian Schindler,
  • Naveen Neradugomma,
  • Winston Thomas,
  • Xiaoyun Liao,
  • Yinhan Zhou,
  • Sean M. West,
  • Feng Wang,
  • Srikanth Kotapati,
  • Guodong Chen,
  • Sayumi Yamazoe,
  • Anastasia Kosenko,
  • Gavin Dollinger,
  • Tim Sproul,
  • Arvind Rajpal,
  • Pavel Strop

DOI
https://doi.org/10.1038/s41598-022-06953-7
Journal volume & issue
Vol. 12, no. 1
pp. 1 – 13

Abstract

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Abstract T-cell engagers (TCEs) are a growing class of biotherapeutics being investigated in the clinic for treatment of a variety of hematological and solid tumor indications. However, preclinical evaluation of TCEs in vivo has been mostly limited to xenograft tumor models in human T-cell reconstituted immunodeficient mice, which have a number of limitations. To explore the efficacy of human TCEs in fully immunocompetent hosts, we developed a knock-in mouse model (hCD3E-epi) in which a 5-residue N-terminal fragment of murine CD3-epsilon was replaced with an 11-residue stretch from the human sequence that encodes for a common epitope recognized by anti-human CD3E antibodies in the clinic. T cells from hCD3E-epi mice underwent normal thymic development and could be efficiently activated upon crosslinking of the T-cell receptor with anti-human CD3E antibodies in vitro. Furthermore, a TCE targeting human CD3E and murine CD20 induced robust T-cell redirected killing of murine CD20-positive B cells in ex vivo hCD3E-epi splenocyte cultures, and also depleted nearly 100% of peripheral B cells for up to 7 days following in vivo administration. These results highlight the utility of this novel mouse model for exploring the efficacy of human TCEs in vivo, and suggest a useful tool for evaluating TCEs in combination with immuno-oncology/non-immuno-oncology agents against heme and solid tumor targets in hosts with a fully intact immune system.