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首页> 美国卫生研究院文献>DNA and Cell Biology >The TCR γδ Repertoire and Relative Gene Expression Characteristics of T-ALL Cases with Biclonal Malignant Vδ1 and Vδ2 T Cells
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The TCR γδ Repertoire and Relative Gene Expression Characteristics of T-ALL Cases with Biclonal Malignant Vδ1 and Vδ2 T Cells

机译:T-ALL恶性Vδ1和Vδ2T细胞病例的TCRγ谱库和相关基因表达特征

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Despite significant improvement in our understanding of T-cell acute lymphoblastic leukemia (T-ALL) biology and pathogenesis, many questions remain unanswered. In previous studies, we found a T-ALL case with two malignant T-cell clones with Vδ1Dδ2Dδ3Jδ1 and Vδ2Dδ3Jδ2 rearrangements. In this study, we further characterized T-ALL cases with two malignant clones containing Vδ1Dδ3Jδ1 and Vδ2Dδ1Jδ1 rearrangements using fine-tiling array comparative genomic hybridization, ligation-mediated polymerase chain reaction (LM-PCR), sequencing, and reverse transcription polymerase chain reaction (RT-PCR) analysis. We further analyzed the distribution and clonality of the T-cell receptor (TCR) Vγ and Vδ subfamily T cells in the two T-ALL cases by RT-PCR and GeneScan. Monoclonal Vδ1 and Vδ2 subfamilies were confirmed in both samples, the Vδ3 through Vδ7 subfamilies could not be detected in the T-ALL samples, whereas the oligoclonal Vδ8 subfamily could be identified. Based on the clinical finding that both of the T-ALL cases with two malignant T-cell clones had a poor outcome, we attempted to compare the expression pattern of genes related to T-cell activation and proliferation between cases with the malignant Vδ1 and Vδ2 T-cell clones and T-ALL cases with a mono-malignant Vα T-cell clone. We selected two T-ALL cases with VαJα rearrangements and analyzed the expression level of Notch1, TAL1, and the CARMA-BCL10-MALT-A20-NF-κB pathway genes by real-time PCR. A20 had significantly higher expression in the biclonal compared with the monoclonal T-ALL group (p=0.0354), and there was a trend toward higher expression for the other genes in the biclonal group with the exception of TAL1, although the differences were not statistically significant. In conclusion, we identified two T-ALL cases with biclonal malignant T-cell clones and described the characteristics of the biclonal T-ALL subtype and its gene expression pattern. Thus, our findings may improve the understanding of biclonal T-ALL.
机译:尽管我们对T细胞急性淋巴细胞白血病(T-ALL)生物学和发病机制的理解有了显着改善,但许多问题仍未得到解答。在先前的研究中,我们发现了一个T-ALL病例,其中有两个恶性T细胞克隆,其中Vδ1Dδ2Dδ3Jδ1和Vδ2Dδ3Jδ2重排。在这项研究中,我们使用精细平铺阵列比较基因组杂交,连接介导的聚合酶链反应(LM-PCR),测序和逆转录聚合酶链式反应(T-ALL)对两个包含Vδ1Dδ3Jδ1和Vδ2Dδ1Jδ1重排的恶性克隆进行了进一步的特征分析RT-PCR)分析。我们通过RT-PCR和GeneScan分析了两个T-ALL病例中T细胞受体(TCR)Vγ和Vδ亚家族T细胞的分布和克隆性。在两个样品中均确认了单克隆Vδ1和Vδ2亚家族,在T-ALL样品中未检测到Vδ3至Vδ7亚家族,而可以鉴定出寡克隆Vδ8亚家族。根据临床发现,两个带有两个恶性T细胞克隆的T-ALL病例均不良预后,我们试图比较具有恶性Vδ1和Vδ2的病例之间与T细胞活化和增殖相关的基因的表达模式T细胞克隆和具有单恶性VαT细胞克隆的T-ALL病例。我们选择了两个VαJα重排的T-ALL病例,并通过实时PCR分析了Notch1,TAL1和CARMA-BCL10-MALT-A20-NF-κB通路基因的表达水平。与单克隆T-ALL组相比,A20在双克隆细胞中的表达明显更高(p = 0.0354),并且在双克隆细胞中,除TAL1外,其他所有基因都有更高表达的趋势,尽管差异无统计学意义重大。总之,我们确定了两例具有双克隆性恶性T细胞克隆的T-ALL病例,并描述了双克隆T-ALL亚型的特征及其基因表达模式。因此,我们的发现可能会增进对双克隆T-ALL的理解。

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