Department of Pathology, Immunology and Laboratory Medicine, Diabetes Institute, College of Medicine, University of Florida, Gainesville, FL, United States.
Department of Molecular Genetics and Microbiology, College of Medicine, University of Florida, Gainesville, FL, United States.
Front Immunol. 2020 Apr 15;11:611. doi: 10.3389/fimmu.2020.00611. eCollection 2020.
The human T lymphocyte compartment is highly dynamic over the course of a lifetime. Of the many changes, perhaps most notable is the transition from a predominantly naïve T cell state at birth to the acquisition of antigen-experienced memory and effector subsets following environmental exposures. These phenotypic changes, including the induction of T cell exhaustion and senescence, have the potential to negatively impact efficacy of adoptive T cell therapies (ACT). When considering ACT with CD4CD25CD127 regulatory T cells (Tregs) for the induction of immune tolerance, we previously reported expanded umbilical cord blood (CB) Tregs remained more naïve, suppressed responder T cells equivalently, and exhibited a more diverse T cell receptor (TCR) repertoire compared to expanded adult peripheral blood (APB) Tregs. Herein, we hypothesized that upon further characterization, we would observe increased lineage heterogeneity and phenotypic diversity in APB Tregs that might negatively impact lineage stability, engraftment capacity, and the potential for Tregs to home to sites of tissue inflammation following ACT. We compared the phenotypic profiles of human Tregs isolated from CB versus the more traditional source, APB. We conducted analysis of fresh and expanded Treg subsets at both the single cell (scRNA-seq and flow cytometry) and bulk (microarray and cytokine profiling) levels. Single cell transcriptional profiles of pre-expansion APB Tregs highlighted a cluster of cells that showed increased expression of genes associated with effector and pro-inflammatory phenotypes (, , and NKG7) with low expression of Treg markers ( and ). CB Tregs were more diverse in TCR repertoire and homogenous in phenotype, and contained fewer effector-like cells in contrast with APB Tregs. Interestingly, expression of canonical Treg markers, such as FOXP3, TIGIT, and IKZF2, were increased in CB CD4CD127 conventional T cells (Tconv) compared to APB Tconv, post-expansion, implying perinatal T cells may adopt a default regulatory program. Collectively, these data identify surface markers (namely CXCR3) that could be depleted to improve purity and stability of APB Tregs, and support the use of expanded CB Tregs as a potentially optimal ACT modality for the treatment of autoimmune and inflammatory diseases.
人类 T 淋巴细胞群在其一生中是高度动态的。在众多变化中,最引人注目的或许是从出生时主要处于幼稚 T 细胞状态向环境暴露后获得抗原经验性记忆和效应亚群的转变。这些表型变化,包括 T 细胞耗竭和衰老的诱导,有可能对过继性 T 细胞治疗(ACT)的疗效产生负面影响。当考虑使用 CD4CD25CD127 调节性 T 细胞(Treg)进行免疫耐受诱导的 ACT 时,我们之前报道过,扩增的脐带血(CB)Treg 仍然更加幼稚,对效应器 T 细胞的抑制作用相当,并且与扩增的成人外周血(APB)Treg 相比,表现出更多样化的 T 细胞受体(TCR)库。在此,我们假设,经过进一步的特征描述,我们将观察到 APB Treg 中增加的谱系异质性和表型多样性,这可能会对谱系稳定性、植入能力以及 Treg 归巢到 ACT 后组织炎症部位的潜力产生负面影响。我们比较了从 CB 与更传统来源 APB 分离的人 Treg 的表型特征。我们在单细胞(scRNA-seq 和流式细胞术)和批量(微阵列和细胞因子谱分析)水平上对新鲜和扩增的 Treg 亚群进行了分析。APB Treg 预扩增的单细胞转录谱突出显示了一群细胞,这些细胞表现出与效应和促炎表型相关的基因表达增加(、和 NKG7),而 Treg 标志物(和)表达降低。与 APB Treg 相比,CB Treg 在 TCR 库中更加多样化,表型更加均一,并且含有较少的效应样细胞。有趣的是,与 APB Tconv 相比,CB CD4CD127 常规 T 细胞(Tconv)中经典 Treg 标志物(如 FOXP3、TIGIT 和 IKZF2)的表达增加,暗示围产期 T 细胞可能采用默认的调节程序。总之,这些数据确定了表面标志物(即 CXCR3),可以通过耗尽这些标志物来提高 APB Treg 的纯度和稳定性,并支持使用扩增的 CB Treg 作为治疗自身免疫和炎症性疾病的潜在最佳 ACT 方式。
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