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首页> 外文期刊>Blood cancer journal. >Lack of common TCRA and TCRB clonotypes in CD8+/TCRαβ+ T-cell large granular lymphocyte leukemia: a review on the role of antigenic selection in the immunopathogenesis of CD8+ T-LGL
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Lack of common TCRA and TCRB clonotypes in CD8+/TCRαβ+ T-cell large granular lymphocyte leukemia: a review on the role of antigenic selection in the immunopathogenesis of CD8+ T-LGL

机译:CD8 + /TCRαβ + T细胞大颗粒淋巴细胞白血病缺乏常见的TCRA和TCRB克隆型:抗原选择在CD8 + T-LGL

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Clonal CD8+/T-cell receptor (TCR)αβ+ T-cell large granular lymphocyte (T-LGL) proliferations constitute the most common subtype of T-LGL leukemia. Although the etiology of T-LGL leukemia is largely unknown, it has been hypothesized that chronic antigenic stimulation contributes to the pathogenesis of this disorder. In the present study, we explored the association between expanded TCR-Vβ and TCR-Vα clonotypes in a cohort of 26 CD8+/TCRαβ+ T-LGL leukemia patients, in conjunction with the HLA-ABC genotype, to find indications for common antigenic stimuli. In addition, we applied purpose-built sophisticated computational tools for an in-depth evaluation of clustering of TCRβ (TCRB) complementarity determining region 3 (CDR3) amino-acid LGL clonotypes. We observed a lack of clear TCRA and TCRB CDR3 homology in CD8+/TCRαβ+ T-LGL, with only low level similarity between small numbers of cases. This is in strong contrast to the homology that is seen in CD4+/TCRαβ+ T-LGL and TCRγδ+ T-LGL and thus underlines the idea that the LGL types have different etiopathogenesis. The heterogeneity of clonal CD8+/TCRαβ+ T-LGL proliferations might in fact suggest that multiple pathogens or autoantigens are involved.
机译:克隆CD8 + / T细胞受体(TCR)αβ + T细胞大颗粒淋巴细胞(T-LGL)增殖是T-LGL白血病最常见的亚型。尽管T-LGL白血病的病因学很大程度上是未知的,但据推测,慢性抗原刺激可导致这种疾病的发病。在本研究中,我们探讨了26名CD8 + /TCRαβ + T-LGL白血病患者队列中扩展的TCR-Vβ与TCR-Vα克隆型之间的关联。结合HLA-ABC基因型,以寻找常见抗原刺激的指征。此外,我们应用了专门构建的复杂计算工具来深入评估TCRβ(TCRB)互补决定区3(CDR3)氨基酸LGL克隆型的聚类。我们观察到在CD8 + /TCRαβ + T-LGL中缺乏清晰的TCRA和TCRB CDR3同源性,少数病例之间只有低水平的相似性。这与CD4 + /TCRαβ + T-LGL和TCRγδ + T-LGL中的同源性形成强烈对比,因此强调了LGL类型具有不同的病因。克隆CD8 + /TCRαβ + T-LGL增殖的异质性实际上可能表明存在多种病原体或自身抗原。

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