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Mechanistic modelling of tyrosine recombination reveals key parameters determining the performance of a CAR T cell switching circuit

机译:酪氨酸重组的力学建模揭示了确定汽车T细胞开关电路性能的关键参数

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摘要

Inducible genetic switches based on tyrosine recombinase-based DNA excision are a promising platform for the regulation and control of chimeric antigen receptor (CAR) T cell activity in cancer immunotherapy. These switches exploit the increased stability of DNA excision in tyrosine recombinases through an inversion-excision circuit design. Here, the authors develop the first mechanistic mathematical model of switching dynamics in tyrosine recombinases and validate it against experimental data through both global optimisation and statistical approximation approaches. Analysis of this model provides guidelines regarding which system parameters are best suited to experimental tuning in order to establish optimal switch performance in vivo. In particular, they find that the switching response can be made significantly faster by increasing the concentration of the inducer drug 4-OHT and/or by using promoters generating higher expression levels of the FlpO recombinase.
机译:基于酪氨酸重组酶的DNA切除的诱导遗传开关是癌症免疫疗法中嵌合抗原受体(CAR)T细胞活性的调控和控制的有希望的平台。这些开关通过反转切除电路设计利用酪氨酸重组酶的DNA切除稳定性增加。在这里,作者通过全局优化和统计近似方法在于,在酪氨酸重组酶中开发了第一个机械数学模型,并通过全局优化和统计近似方法对实验数据进行验证。对该模型的分析提供了关于哪些系统参数最适合实验调整的指导方针,以便在体内建立最佳的开关性能。特别地,他们发现通过增加诱导剂4-OHT和/或通过使用产生更高表达水平的FLPO重组酶的促进剂的启动子来制备切换响应。

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