多功能Tbet T细胞对慢性淋巴细胞白血病特定临床事件的影响。
Influence of polyfunctional Tbet T cells on specific clinical events in chronic lymphocytic leukaemia.
作者信息
Lim Yeong Jer, Duckworth Andrew D, Clarke Kim, Kennedy Paul, Karpha Indrani, Oates Melanie, Gornall Matthew, Kalakonda Nagesh, Slupsky Joseph R, Pettitt Andrew R
机构信息
Department of Molecular & Clinical Cancer Medicine, University of Liverpool, Liverpool, United Kingdom.
Haemato-oncology Department, The Clatterbridge Cancer Centre National Health Service (NHS) Foundation Trust, Liverpool, United Kingdom.
出版信息
Front Immunol. 2025 Apr 17;16:1528405. doi: 10.3389/fimmu.2025.1528405. eCollection 2025.
INTRODUCTION
T-cell dysfunction is a hallmark of chronic lymphocytic leukemia (CLL), but the extent to which individual CD4 or CD8 T-cell subpopulations influence specific clinical events remains unclear. To address this knowledge gap, we utilised high-dimensional mass cytometry to profile circulating CD4 and CD8 T-cells in pre-treatment samples from a well-defined cohort of CLL patients undergoing initial therapy as part of a clinical trial.
METHODS
Pre-treatment blood samples from 138 CLL patients receiving initial chemoimmunotherapy containing bendamustine or chlorambucil in the NCRI RIAltO trial (NCT01678430; EudraCT 2011-000919-22) were subjected to deep immunophenotyping by mass cytometry using a bespoke panel of 37 antibodies. T-cell clusters were identified through unsupervised clustering and related to treatment outcomes. Additionally, a randomly selected cohort of 30 CLL patients underwent T-cell stimulation with anti-CD3/CD28 microbeads, followed by cytokine analysis using a separate 36-antibody panel, which included seven cytokines.
RESULTS
Seventeen CD4 and 22 CD8 T-cell clusters were identified in a discovery cohort of 79 patients. Three of these clusters, measured as a proportion of their parental CD4 or CD8 populations, correlated with a reduced risk of grade ≥3 infection, grade ≥3 second primary malignancy (SPM) and death, respectively. Three corresponding T-cell subpopulations prospectively defined by non-redundant markers and Boolean gating (ICOSHLA-DRPD1TIGITTbetCD4 T-helper cells; CD27CD28-PD1TbetEomesCD8 cells; and CD27CD28-GrymBTbetEomesCD8 terminal effector cells) showed the same clinical correlations as the clusters on which they were based. With the exception of SPM for which there were insufficient events, these correlations were confirmed in a separate validation cohort of 59 patients. stimulation of a subset of CLL patients in the discovery cohort showed an enrichment of primed and polyfunctional cells in all three Tbet T-cell subpopulations of interest.
CONCLUSION
Our study provides new insights into the potential for Tbet+ T-cell subpopulations to influence and predict specific clinical events in CLL. This, in turn, raises the possibility that these respective subpopulations could play an important role in controlling infection, solid tumours and CLL itself.
CLINICAL TRIAL REGISTRATION
https://www.clinicaltrials.gov/, identifier NCT01678430; https://www.isrctn.com/ISRCTN09988575, identifier EudraCT 2011-000919-22.
引言
T细胞功能障碍是慢性淋巴细胞白血病(CLL)的一个标志,但单个CD4或CD8 T细胞亚群对特定临床事件的影响程度仍不清楚。为了填补这一知识空白,我们利用高维质谱流式细胞术对一组明确的CLL患者在初始治疗前的样本中的循环CD4和CD8 T细胞进行分析,这些患者作为一项临床试验的一部分正在接受初始治疗。
方法
在NCRI RIAltO试验(NCT01678430;EudraCT 2011-000919-22)中,对138例接受含苯达莫司汀或苯丁酸氮芥的初始化疗免疫治疗的CLL患者的治疗前血样,使用一组定制的37种抗体通过质谱流式细胞术进行深度免疫表型分析。通过无监督聚类识别T细胞簇,并将其与治疗结果相关联。此外,随机选择30例CLL患者组成队列,用抗CD3/CD28微珠刺激T细胞,随后使用一个单独的包含7种细胞因子的36抗体面板进行细胞因子分析。
结果
在一个由79例患者组成的发现队列中,鉴定出17个CD4和22个CD8 T细胞簇。这些簇中的三个,以其亲本CD4或CD8群体的比例衡量,分别与≥3级感染、≥3级第二原发性恶性肿瘤(SPM)和死亡风险降低相关。通过非冗余标记和布尔门控前瞻性定义的三个相应T细胞亚群(ICOSHLA-DRPD1TIGITTbetCD4辅助性T细胞;CD27CD28-PD1TbetEomesCD8细胞;以及CD27CD28-GrymBTbetEomesCD8终末效应细胞)显示出与它们所基于的簇相同的临床相关性。除了SPM事件不足外,这些相关性在另一个由59例患者组成的验证队列中得到证实。对发现队列中的一部分CLL患者进行刺激后发现,在所有三个感兴趣的Tbet T细胞亚群中,启动细胞和多功能细胞都有所富集。
结论
我们的研究为Tbet+ T细胞亚群影响和预测CLL中特定临床事件的潜力提供了新的见解。这反过来又增加了这些各自的亚群可能在控制感染、实体瘤和CLL本身方面发挥重要作用的可能性。
临床试验注册
https://www.clinicaltrials.gov/,标识符NCT01678430;https://www.isrctn.com/ISRCTN09988575,标识符EudraCT 2011-000919-22。
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