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Human effector CD8+ T cells derived from naive rather than memory subsets possess superior traits for adoptive immunotherapy

机译:源自幼稚而非记忆亚群的人类效应CD8 + T细胞具有过继免疫疗法的优良特性

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摘要

Cluster of differentiation (CD)8+ T cells exist as naive, central memory, and effector memory subsets, and any of these populations can be genetically engineered into tumor-reactive effector cells for adoptive immunotherapy. However, the optimal subset from which to derive effector CD8+ T cells for patient treatments is controversial and understudied. We investigated human CD8+ T cells and found that naive cells were not only the most abundant subset but also the population most capable of in vitro expansion and T-cell receptor transgene expression. Despite increased expansion, naive-derived cells displayed minimal effector differentiation, a quality associated with greater efficacy after cell infusion. Similarly, the markers of terminal differentiation, killer cell lectin-like receptor G1 and CD57, were expressed at lower levels in cells of naive origin. Finally, naive-derived effector cells expressed higher CD27 and retained longer telomeres, characteristics that suggest greater proliferative potential and that have been linked to greater efficacy in clinical trials. Thus, these data suggest that naive cells resist terminal differentiation, or “exhaustion,” maintain high replicative potential, and therefore may be the superior subset for use in adoptive immunotherapy.
机译:分化(CD)8+ T细胞簇以幼稚,中枢记忆和效应记忆子集的形式存在,这些群体中的任何一个都可以通过基因工程改造成对肿瘤具有反应性的效应细胞进行过继免疫治疗。然而,从中获得用于患者治疗的效应CD8 + T细胞的最佳子集是有争议的,并且尚未得到研究。我们研究了人类CD8 + T细胞,发现幼稚细胞不仅是最丰富的子集,而且是最有能力在体外扩增和T细胞受体转基因表达的人群。尽管扩增增加,但幼稚来源的细胞显示出最小的效应子分化,这种质量与细胞输注后的更高功效有关。同样,终末分化的标志物,杀伤细胞凝集素样受体G1和CD57,在幼稚来源的细胞中以较低的水平表达。最后,幼稚的效应细胞表达更高的CD27并保留更长的端粒,这些特征表明具有更大的增殖潜力,并且在临床试验中与更高的功效有关。因此,这些数据表明,幼稚细胞抵抗终末分化或“精疲力竭”,具有很高的复制潜力,因此可能是过继免疫疗法中的优势子集。

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