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体外诱导抗白血病 T 细胞的反应模式:通过光谱分析和免疫表型分析进行特征描述。

In vitro-induced response patterns of antileukemic T cells: characterization by spectratyping and immunophenotyping.

机构信息

Faculty of Medical, Department of Paediatric Oncology, Haematology and Immunology, University Dusseldorf, 40225, Dusseldorf, Germany.

出版信息

Clin Exp Med. 2013 Feb;13(1):29-48. doi: 10.1007/s10238-012-0180-y. Epub 2012 Mar 23.

DOI:10.1007/s10238-012-0180-y
PMID:22441559
Abstract

Myeloid leukemic cells can be induced to differentiate into leukemia-derived dendritic cells (DCleu) regaining the stimulatory capacity of professional DCs while presenting the leukemic antigen repertoire. But so far, the induced antileukemic T-cell responses are variable both in specificity and in efficacy. In an attempt to elucidate the underlying causes of different T-cell response patterns, T-cell receptor (TR) Vβ chain rearrangements were correlated with the T cells corresponding immunophenotypic profile, as well as their proliferative response and cytolytic capacities. In three different settings, donor T cells, either human leukocyte antigen matched or mismatched (haploidentical), or autologous T cells were repeatedly stimulated with myeloid blasts or leukemia-derived DC/DCleus from the corresponding patients diseased from acute myeloid leukemia (AML). Although no significant differences in T-cell proliferation were observed, the T-cell-mediated cytolytic response pattern varied considerably and even caused blast proliferation in two cases. Spectratyping revealed a remarkable restriction (>75% of normal level) of the CD4+ or CD8+-TR repertoire of blast- or DC/DCleu-stimulated T cells. Although in absolute terms, DC/DCleu stimulation induced the highest grade of restriction in the CD8+ T-cell subset, the CD4+ T-cell compartment seemed to be relatively more affected. But most importantly, in vitro stimulation with DC/DCleu resulted into an identical TR restriction pattern (β chain) that could be identified in vivo in a patient sample 3 months after allo-SCT. Thus, in vitro tests combining functional flow cytometry with spectratyping might provide predictive information about T cellular response patterns in vivo.

摘要

髓系白血病细胞可被诱导分化为白血病衍生树突状细胞(DCleu),在恢复专业树突状细胞的刺激能力的同时,呈现白血病抗原库。但到目前为止,诱导的抗白血病 T 细胞反应在特异性和疗效方面都存在差异。为了阐明不同 T 细胞反应模式的潜在原因,T 细胞受体(TR)Vβ 链重排在与 T 细胞相应的免疫表型特征、增殖反应和细胞溶解能力相关的同时,也进行了分析。在三种不同的情况下,供体 T 细胞(人类白细胞抗原匹配或不匹配(单倍体)或自体 T 细胞)反复用髓样母细胞或来自相应患有急性髓系白血病(AML)的患者的白血病衍生 DC/DCleu 刺激。尽管 T 细胞增殖没有观察到显著差异,但 T 细胞介导的细胞溶解反应模式差异很大,甚至在两种情况下导致母细胞增殖。谱分析显示,母细胞或 DC/DCleu 刺激的 T 细胞的 CD4+或 CD8+-TR 库受到显著限制(>正常水平的 75%)。尽管在绝对值方面,DC/DCleu 刺激在 CD8+T 细胞亚群中诱导的限制程度最高,但 CD4+T 细胞区室似乎受到的影响相对较大。但最重要的是,体外用 DC/DCleu 刺激导致在同种异体 SCT 后 3 个月患者样本中可识别的体内相同的 TR 限制模式(β链)。因此,体外测试将功能流式细胞术与谱分析相结合,可能提供体内 T 细胞反应模式的预测信息。

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