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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Soluble and membrane levels of molecules involved in the interaction between clonal plasma cells and the immunological microenvironment in multiple myeloma and their association with the characteristics of the disease.
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Soluble and membrane levels of molecules involved in the interaction between clonal plasma cells and the immunological microenvironment in multiple myeloma and their association with the characteristics of the disease.

机译:多克隆性骨髓瘤中克隆浆细胞与免疫微环境相互作用的分子的可溶性和膜水平及其与疾病特征的关系。

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Clonal plasma cells (PC) from different types of monoclonal gammopathies (MG) display distinct phenotypes consistent with an increased antigen-presentation and T-cell costimulation in MG of undetermined significance that deteriorates in malignant conditions. Expression of other cell surface and soluble molecules (e.g. adhesion/proliferation molecules) involved in the interaction between clonal PC and the bone marrow (BM) microenvironment has also been related to malignant PC, although the exact clinical significance of their expression remains largely unknown. Analysis of cell surface levels of several of these molecules in multiple myeloma (MM) patients shows an association between lower expression on BMPC of the HLA-I and beta2-microglobulin antigen-presenting molecules, the CD126 and CD130 IL6 receptor (IL6R) chains, and CD38, and adverse prognostic features of the disease. Likewise, patients showing higher soluble levels of antigen-presenting molecules (HLA-I and beta2-microglobulin), IL6R and CD95tended to be associated with more aggressive disease behavior. In contrast, CD40, CD86, CD56, CD19, and CD45 were not associated with patients' outcome. Interestingly, upon considering the ratio between the soluble and PC membrane expression of each molecule, an increased adverse prognostic impact was observed for both HLA-I and beta2-microglobulin, but not for the other molecules. Multivariate analysis confirmed the independent prognostic value of cell surface expression of CD126 on BMPC together with serum beta2-microglobulin and LDH. In summary, our results show an abnormal distribution of the cellular and soluble compartments of the HLA-I, IL6R, and to a lower extent, CD95 molecules, in MM, associated with the clinical characteristics and behavior of the disease.
机译:来自不同类型的单克隆变态反应(MG)的克隆浆细胞(PC)显示出不同的表型,这与MG中抗原呈递和T细胞共刺激性的增加相一致,而其不确定性却在恶性条件下恶化。参与克隆PC和骨髓(BM)微环境相互作用的其他细胞表面和可溶性分子(例如黏附/增殖分子)的表达也与恶性PC有关,尽管其表达的确切临床意义仍然未知。对多发性骨髓瘤(MM)患者中这些分子中的几种分子的细胞表面水平的分析表明,HLA-1和β2-微球蛋白抗原呈递分子在CDPC上的低表达与CD126和CD130 IL6受体(IL6R)链之间存在关联,和CD38,以及该疾病的不良预后特征。同样,表现出较高可溶性水平的抗原呈递分子(HLA-1和β2-微球蛋白),IL6R和CD95的患者倾向于与更具侵略性的疾病行为相关。相反,CD40,CD86,CD56,CD19和CD45与患者的预后无关。有趣的是,考虑到每个分子的可溶性膜和PC膜表达之间的比率,HLA-1和β2-微球蛋白的不良预后影响都增加了,而其他分子则没有。多变量分析证实了BMPC上CD126细胞表面表达以及血清β2-微球蛋白和LDH的独立预后价值。总而言之,我们的结果显示MM中HLA-1,IL6R的细胞和可溶性区室异常分布,以及CD95分子在较低程度上与疾病的临床特征和行为有关。

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