DAP12-associated synthetic antigen receptors enable multi-targeting of T cells with independent chimeric receptors in a small genetic payload

IF 4.1 2区综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES iScience Pub Date : 2025-03-07 DOI:10.1016/j.isci.2025.112142

Allyson E. Moore , Hayley Nault , Derek Cummings , Bonnie Bojovic , Nick Serniuck , Christopher L. Baker , Craig Aarts , Chitra Venugopal , Sheila K. Singh , Joanne A. Hammill , Jonathan L. Bramson

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Abstract

We describe a series of DAP12-associated receptors that can be used to achieve multi-targeting within a small genetic payload. Empirical evaluation of scaffold/binder combinations is required to define the optimal synthetic receptor configuration. When two DAP12-associated synthetic receptors were expressed in T cells from a single vector, the surface levels of individual receptors was reduced when compared to T cells engineered with vectors that express a single receptor. The reduction in receptor expression had a pronounced effect on early, but not late, signaling events and primarily affected cytokine production. The functional deficiency was overcome by increasing synthetic receptor levels demonstrating that there is no fundamental issue related to co-expression of multiple DAP12-associated synthetic receptors in a single T cell. Our data show that T cells can be engineered with multiple recombinant DAP12-based receptors to yield multi-target specific T cells, however, thoughtful design and optimization are necessary.

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dap12相关的合成抗原受体能够在一个小的遗传载荷中使用独立的嵌合受体靶向T细胞

我们描述了一系列dap12相关受体，可用于在小遗传有效载荷内实现多靶向。需要对支架/粘合剂组合进行经验评估，以确定最佳的合成受体配置。当两个dap12相关的合成受体通过单一载体在T细胞中表达时，与表达单一受体的载体工程T细胞相比，单个受体的表面水平降低。受体表达的减少对早期而非晚期的信号事件有显著影响，并主要影响细胞因子的产生。通过增加合成受体水平克服了功能缺陷，这表明在单个T细胞中不存在与多个dap12相关合成受体共表达相关的根本问题。我们的数据表明，T细胞可以用多种重组dap12受体进行工程设计，以产生多靶点特异性T细胞，但需要深思熟虑的设计和优化。

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来源期刊

iScience Multidisciplinary-Multidisciplinary

CiteScore

7.20

自引率

1.70%

发文量

1972

审稿时长

6 weeks

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