SOLUBLE CD150 ISOFORM LEVEL IN PLASMA OF CHRONIC LYMPHOCYTIC LEUKEMIA PATIENTS.

I Gordiienko, V Shcherbina, L Shlapatska
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Abstract

Background: SLAMF1/CD150 is an active player in B cell signaling networks in chronic lymphocytic leukemia (CLL). CD150-mediated signaling initiates through a homophilic CD150 binding, which spans the adjacent cells, or the interaction with the soluble CD150 isoform (sCD150). The expression of sCD150 isoform at the mRNA and protein levels ex vivo was confirmed. However, it is unclear whether sCD150 isoform present in the blood plasma of CLL patients is a factor in the constitutive activation of CD150+ cells. The aim of this study was to develop an ELISA assay for the specific sCD150 evaluation and assess the sCD150 levels in the blood plasma of CLL patients with different CD150 expression on B cells.

Materials and methods: Blood plasma samples and peripheral blood mononuclear cells from 40 previously untreated CLL patients were analyzed. An ELISA method, ex vivo drug sensitivity assay, and a cell viability assay were used.

Results: The sCD150 isoform was found in all studied plasma samples of CLL patients at different levels regardless of the cell surface CD150 expression status of B cells and sCD150 mRNA expression. CLL cases with low levels of the cell surface CD150 expression in B cells are characterized by high levels of sCD150 in blood plasma in contrast to the CLL cases with high cell surface CD150 expression on B cells. The elevated levels of sCD150 in blood plasma are associated with a better sensitivity of malignant B cells to cyclophosphamide and bendamustine.

Conclusions: The sCD150 isoform is actively secreted by CLL B cells with its accumulation in blood plasma, which may be regarded as an additional factor in the CLL clinicopathologic variability.

慢性淋巴细胞白血病患者血浆中可溶性 cd150 同工酶水平。
背景:SLAMF1/CD150是慢性淋巴细胞白血病(CLL)B细胞信号网络中的活跃分子。CD150介导的信号传导是通过跨越邻近细胞的同嗜性CD150结合或与可溶性CD150异构体(sCD150)的相互作用启动的。sCD150 异构体在体内外 mRNA 和蛋白质水平的表达已得到证实。然而,尚不清楚CLL患者血浆中的sCD150异构体是否是CD150+细胞构成性活化的一个因素。本研究的目的是开发一种用于特异性评估 sCD150 的酶联免疫吸附试验,并评估 B 细胞上 CD150 表达不同的 CLL 患者血浆中的 sCD150 水平:分析了40名既往未经治疗的CLL患者的血浆样本和外周血单核细胞。采用酶联免疫吸附法、体内外药物敏感性检测法和细胞活力检测法:结果:在所有研究的 CLL 患者血浆样本中都发现了不同水平的 sCD150 异构体,与 B 细胞的细胞表面 CD150 表达状态和 sCD150 mRNA 表达无关。B细胞细胞表面CD150表达水平低的CLL病例血浆中sCD150水平高,而B细胞细胞表面CD150表达水平高的CLL病例血浆中sCD150水平低。血浆中sCD150水平的升高与恶性B细胞对环磷酰胺和苯达莫司汀更敏感有关:sCD150异构体由CLL B细胞主动分泌,并在血浆中蓄积,这可能被视为CLL临床病理变异的另一个因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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