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可溶性人类白细胞抗原-G(sHLA-G)血浆水平以及信使HLA-G在B细胞慢性淋巴细胞白血病(B-CLL)中的意义。

The significance of soluble HLA-G plasma levels as well as messenger HLA-G for B-cell chronic lymphocytic leukemia (B-CLL).

作者信息

Giannopoulos K, Schmitt M, Kowal M, Własiuk P, Bojarska-Junak A, Roliński J, Dmoszyńska A

机构信息

Clinical Immunology Department, Medical University of Lublin, Lublin, Poland.

出版信息

Leuk Res. 2008 Dec;32(12):1815-9. doi: 10.1016/j.leukres.2008.04.008. Epub 2008 May 21.

Abstract

The immunosuppression accompanies B-cell chronic lymphocytic leukemia (B-CLL) but might be also responsible for disease progression by enabling CLL cells to escape from the immunosurveillance. Some particles involved in the regulation of an immune system might represent prognostic value for B-CLL. Recently we found no correlation between HLA-G on messenger and protein level, suggesting that HLA-G is released in soluble form. To confront this hypothesis we characterized soluble HLA-G (sHLA-G) by the prognostic factors in the first cohort of 34 CLL patients. No correlation was observed between sHLA-G levels in ZAP-70(+) and ZAP-70(-) CLL as well as in CD38(+) CLL and CD38(-) CLL patients. Next, we wondered whether gene expression of HLA-G, which represent the whole HLA-G pool in the cell, posses prognostic value for CLL. In the second cohort of 41 CLL patients we assessed messenger levels of HLA-G by the strongest prognostic factors in CLL including cytogenetics, IgVH mutational status, ZAP-70 as well as CD38. No changes of HLA-G expression levels were found in different CLL groups characterized by IgVH gene mutational status, ZAP-70 as well as CD38. We observed no differences in expression of HLA-G in various cytogenetic groups of CLL including del17p, del13q, del11q, +8q, +3q, del14q and del6q when compared to those with normal karyotype or with 12+. Both, mRNA expression of HLA-G and levels of its soluble form in plasma bring no additional prognostic value for B-CLL patients.

摘要

免疫抑制伴随着B细胞慢性淋巴细胞白血病(B-CLL),但也可能通过使CLL细胞逃避免疫监视而导致疾病进展。一些参与免疫系统调节的颗粒可能对B-CLL具有预后价值。最近我们发现信使水平和蛋白水平上的HLA-G之间没有相关性,这表明HLA-G是以可溶性形式释放的。为了验证这一假设,我们在首批34例CLL患者中根据预后因素对可溶性HLA-G(sHLA-G)进行了特征分析。在ZAP-70(+)和ZAP-70(-)的CLL患者以及CD38(+)和CD38(-)的CLL患者中,未观察到sHLA-G水平之间的相关性。接下来,我们想知道代表细胞中整个HLA-G库的HLA-G基因表达是否对CLL具有预后价值。在第二批41例CLL患者中,我们根据CLL中最强的预后因素评估了HLA-G的信使水平,这些因素包括细胞遗传学、IgVH突变状态、ZAP-70以及CD38。在以IgVH基因突变状态、ZAP-70以及CD38为特征的不同CLL组中,未发现HLA-G表达水平有变化。与核型正常或有12+的患者相比,我们在包括del17p、del13q、del11q、+8q、+3q、del14q和del6q在内的各种CLL细胞遗传学组中未观察到HLA-G表达的差异。HLA-G的mRNA表达及其血浆中可溶性形式的水平均未给B-CLL患者带来额外的预后价值。

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