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The Construction of Chimeric T-Cell Receptor with Spacer Base of Modeling Study of VHH and MUC1 Interaction

机译:VHH和MUC1相互作用模型研究的间隔基嵌合T细胞受体的构建

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摘要

Adaptive cell immunotherapy with the use of chimeric receptors leads to the best and most specific response against tumors. Chimeric receptors consist of a signaling fragment, extracellular spacer, costimulating domain, and an antibody. Antibodies cause immunogenicity; therefore, VHH is a good replacement for ScFv in chimeric receptors. Since peptide sequences have an influence on chimeric receptors, the effect of peptide domains on each other's conformation were investigated. CD3Zeta, CD28, VHH and CD8α, and FcgIIα are used as signaling moieties, costimulating domain, antibody, and spacers, respectively. To investigate the influence of the ligation of spacers on the conformational structure of VHH, models of VHH were constructed. Molecular dynamics simulation was run to study the influence of the presence of spacers on the conformational changes in the binding sites of VHH. Root mean square deviation and root mean square fluctuation of critical segments in the binding site showed no noticeable differences with those in the native VHH. Results from molecular docking revealed that the presence of spacer FcgIIα causes an increasing effect on VHH with MUC1 interaction. Each of the constructs was transformed into the Jurkat E6.1. Expression analysis and evaluation of their functions were examined. The results showed good expression and function.
机译:使用嵌合受体的自适应细胞免疫疗法可导致针对肿瘤的最佳和最特异性反应。嵌合受体由信号片段,细胞外间隔子,共刺激结构域和抗体组成。抗体引起免疫原性;因此,VHH是嵌合受体中ScFv的良好替代品。由于肽序列对嵌合受体有影响,因此研究了肽结构域对彼此构象的影响。 CD3Zeta,CD28,VHH和CD8α和FcgIIα分别用作信号传导部分,共刺激结构域,抗体和间隔区。为了研究间隔基的连接对VHH的构象结构的影响,构建了VHH模型。进行分子动力学模拟以研究间隔物的存在对VHH结合位点构象变化的影响。结合位点关键节段的均方根偏差和均方根波动与天然VHH相比无明显差异。分子对接的结果表明,间隔子FcgIIα的存在对具有MUC1相互作用的VHH的作用增加。每个构造都转换为Jurkat E6.1。进行了表达分析和功能评估。结果显示了良好的表达和功能。

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