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Differential and tumor-specific expression of CD160 in B-cell malignancies

机译:CD160在B细胞恶性肿瘤中的差异表达和肿瘤特异性表达

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摘要

CD160 is a human natural killer (NK)-cell–activating receptor that is also expressed on T-cell subsets. In the present study, we examined 811 consecutive cases of B-cell lymphoproliferative disorders (B-LPDs), and demonstrated CD160 expression in 98% (590 of 600) of chronic lymphocytic leukemia (CLL) cases, 100% (32 of 32) of hairy cell leukemia (HCL) cases, 15% (5 of 34) of mantle cell lymphoma (MCL) in the leukemic phase, and 16% (23 of 145) of other B-LPD cases. CD160 transcript and protein were absent in the normal B-cell hierarchy, from stem cells, B-cell precursors, maturing B cells in the germinal center, and circulating B cells, including CD5+CD19+ B1 cells in umbilical cord. CD160 positivity was significantly higher in CLL and HCL in terms of percentage (65.9% and 67.8%, respectively, P < .0001) and median fluorescence intensity (552 and 857, respectively, P < .0001) compared with all other B-LPD cases. Lymph node CLL samples were also CD160+. Using the disease-specific expression of CD5, CD23, and CD160, a score of 3 characterized CLL (diagnostic odds ratio, 1430); a score of 0 excluded CLL, MCL, and HCL; and the CD23/CD5 ratio differentiated CLL from leukemic CD23+ MCL. In the B-cell lineage, CD160 is a tumor-specific antigen known to mediate cellular activation signals in CLL, and is a novel target for therapeutic manipulation and monitoring of minimal residual disease.
机译:CD160是人类自然杀伤(NK)细胞激活受体,也在T细胞亚群上表达。在本研究中,我们检查了811例连续的B细胞淋巴增生性疾病(B-LPDs),并证明了98%(600例中的590例)慢性淋巴细胞性白血病(CLL),100%(32例中的32例)的CD160表达的毛发性白血病(HCL)病例占15%(34个中的5个)处于白血病期的套细胞淋巴瘤(MCL),其他B-LPD病例的16%(145个中的23个)。干细胞,B细胞前体细胞,生发中心中成熟的B细胞和循环B细胞(包括CD5 + CD19 )在正常B细胞​​层次中均不存在CD160转录本和蛋白质。脐带中的+ B1细胞。与其他B-LPD相比,CLL和HCL中的CD160阳性率(分别为百分比(分别为65.9%和67.8%,P <.0001)和中值荧光强度(分别为552和857,P <.0001)更高)案件。淋巴结CLL样本也为CD160 + 。使用CD5,CD23和CD160的疾病特异性表达,得分为3的特征性CLL(诊断优势比为1430);排除CLL,MCL和HCL的得分为0; CD23 / CD5比值将CLL与白血病CD23 + MCL区分开。在B细胞谱系中,CD160是一种已知的肿瘤特异性抗原,可介导CLL中的细胞激活信号,并且是治疗性操作和监测最小残留疾病的新型靶标。

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