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2DGE and DIGE based proteomic study of malignant B-cells in B-cell acute lymphoblastic leukemia

机译:基于2DGE和DIGE的B细胞急性淋巴细胞白血病恶性B细胞蛋白质组学研究

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With an objective of defining potential diagnostic and/or therapeutic markers and the mechanism of cellular transformation, we present a comparative proteomic study of B-lymphocytes from B-cell acute lymphoblastic leukemia (B-ALL) patients and normal controls, using two-dimensional gel electrophoresis and MALDI ToF/ToF tandem mass spectrometry. Our study led to the identification of 79 differentially regulated proteins in the malignant cells including proteins participating in proteostasis, cytoskeletal organization, redox homeostasis, and signal transduction pathways relevant to leukemogenesis. Principal component analysis displayed immunophenotype-/genotype-dependent variations in the malignant cell proteome. Our study adds new insights to the leukemogenic B-cell biology and prognostic stratifications.
机译:为了定义潜在的诊断和/或治疗标志物以及细胞转化的机制,我们使用二维方法,对来自B细胞急性淋巴细胞白血病(B-ALL)患者和正常对照的B淋巴细胞进行蛋白质组学比较研究凝胶电泳和MALDI ToF / ToF串联质谱分析。我们的研究导致在恶性细胞中鉴定出79种差异调节蛋白,包括参与蛋白稳态,细胞骨架组织,氧化还原稳态和与白血病生成相关的信号转导途径的蛋白质。主成分分析显示恶性细胞蛋白质组中免疫表型/基因型依赖性变异。我们的研究为致白血病的B细胞生物学和预后分层增加了新的见解。

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