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首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Addition of the C-terminus of CD6 to a chimeric antigen receptor enhances cytotoxicity and does not compromise expression
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Addition of the C-terminus of CD6 to a chimeric antigen receptor enhances cytotoxicity and does not compromise expression

机译:添加CD6的C-末端至嵌合抗原受体增强了细胞毒性并且不会妥协表达

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摘要

T cells expressing chimeric antigen receptors (CARs) are a promising new cancer immunotherapy that has now reached the clinic. CARs are synthetic receptors that redirect T cells towards a tumour-associated antigen and activate them through various fused signalling regions, for example derived from CD3 zeta, 4-1BB or CD28. Analysis of the optimal combination of CAR components including signalling domains is not yet comprehensive and may vary with the particular application. The C-terminus of the T-cell surface receptor CD6 is critical for its co-stimulatory effects and signals through two phospho-tyrosine motifs that bind to the intracellular adaptor proteins GADS and SLP-76. Addition of the C terminus of CD6 did not compromise CAR expression, showing it was a stable moiety that can be used independently of the native receptor. A third-generation CAR containing 4-1BB, CD3 zeta and the C terminus of CD6 (4-1BBz-CD6) enhanced interferon-gamma release and cytotoxicity when compared with the second-generation 4-1BB CD3 zeta (4-1BBz) CAR. The CD6 C terminus is a valuable addition to potential components for modular design of CARs to improve effector function, particularly cytotoxicity.
机译:表达嵌合抗原受体(汽车)的T细胞是现有的新癌症免疫疗法,现已到达诊所。汽车是合成受体,其将T细胞重定向肿瘤相关的抗原并通过各种熔化的信号区激活它们,例如衍生自CD3 Zeta,4-1bb或CD28。分析包括信令域的汽车成分的最佳组合尚未综合,并且可能因特定应用而变化。 T细胞表面受体CD6的C-末端对于其共刺激效应和信号通过与细胞内衔接子GAD和SLP-76结合的两种磷酸酪氨酸基序。添加CD6的C末端并未损害轿厢表达,显示它是可以独立于天然受体使用的稳定部分。与第二代4-1BB CD3 Zeta(4-1BBZ)汽车相比,含有4-1BB,CD3 Zeta和CD6(4-1bbz-CD6)的C末端的CD6(4-1bbz-CD6)的C末端和细胞毒性。 CD6 C Terminus是对汽车模块化设计的潜在组件的有价值的补充,以改善效应功能,特别是细胞毒性。

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