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Transformation of mature mouse B cells into malignant plasma cells in vitro via introduction of defined genetic elements

机译:成熟的小鼠B细胞转变成通过介绍恶性浆细胞体外定义遗传元素

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Abstract An experimental system where defined alterations in gene function or gene expression levels in primary B cells would result in the development of transformed plasma cells in vitro would be useful in order to facilitate studies of the underlying molecular mechanisms of plasma cell malignancies. Here, such a system is described in which primary murine B cells rapidly become transformed into surface CD138 + , IgM ?/low , CD19 ? IgM‐secreting plasma cells as a result of expression of the transcription factors IRF4 and MYC together with simultaneous expression of BMI1, mutated p53 or silencing of p19 Arf , and suppression of intrinsic apoptosis through expression of BCLXL. Analysis of gene expression patterns revealed that this combination of transforming genes resulted in expression of a number of genes previously associated with terminally differentiated B cells (plasma cells) and myeloma cells, whereas many genes associated with mature B cells and B‐cell lymphomas were not expressed. Upon transplantation, the transformed cells preferentially localized to the bone marrow, presenting features of a plasma cell malignancy of the IgM isotype. The present findings may also be applicable in the development of novel methods for production of monoclonal antibodies.
机译:抽象的实验系统中定义基因功能或基因表达的改变会导致在初级B细胞水平转换后的浆细胞体外的发展为了方便有用的研究等离子体的潜在的分子机制细胞的恶性肿瘤。描述主要的小鼠B细胞迅速成为转化成表面CD138 +, IgM? /低,CD19 ?转录因子的表达的结果IRF4 MYC一起同步表达BMI1, p53突变或沉默p19 Arf,固有细胞凋亡的抑制通过BCLXL的表情。表达模式显示改变基因导致的组合许多基因的表达与B细胞终末分化有关(浆细胞)和骨髓瘤细胞,而很多与成熟相关的基因B细胞和B细胞淋巴瘤是不表达。转化细胞移植优先局部骨髓,浆细胞恶性肿瘤的特征IgM的同形像。适用小说发展的方法单克隆抗体的生产。

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