Ma A, Fisher P, Dildrop R, Oltz E, Rathbun G, Achacoso P, Stall A, Alt F W
Howard Hughes Medical Institute, Boston, MA.
EMBO J. 1992 Jul;11(7):2727-34. doi: 10.1002/j.1460-2075.1992.tb05338.x.
Transgenic mice carrying either the c-myc or N-myc oncogene deregulated by the immunoglobulin heavy chain enhancer element (E mu) develop both pre-B and B cell lymphomas (E mu-c-myc and E mu-N-myc lymphomas). We report here that B cell lines derived from these tumors, as well as a line derived from v-myc retroviral transformation, simultaneously express surface immunoglobulin (a hallmark of mature B cells) as well as a common subset of genes normally restricted to the pre-B stage of development-including the recombinase activating genes RAG-1 and RAG-2. Continued RAG-1 and RAG-2 expression in these lines is associated with VDJ recombinase activity detected with a VDJ recombination substrate. Cross-linking of the surface immunoglobulin on these lines with an anti-mu antibody leads to rapid, specific and reversible down-regulation of RAG-1 and RAG-2 gene expression. We also find that a small but significant percentage of normal surface immunoglobulin bearing bone marrow B cells express the RAG-1 gene. These findings are discussed in the context of their possible implications for the control of specific gene expression during the pre-B to B cell transition.
携带由免疫球蛋白重链增强子元件(Eμ)失调的c-myc或N-myc癌基因的转基因小鼠会发生前B细胞和B细胞淋巴瘤(Eμ-c-myc和Eμ-N-myc淋巴瘤)。我们在此报告,源自这些肿瘤的B细胞系以及源自v-myc逆转录病毒转化的细胞系,同时表达表面免疫球蛋白(成熟B细胞的一个标志)以及通常仅限于发育前B阶段的一组共同基因,包括重组激活基因RAG-1和RAG-2。这些细胞系中RAG-1和RAG-2的持续表达与用VDJ重组底物检测到的VDJ重组酶活性相关。用抗μ抗体使这些细胞系上的表面免疫球蛋白交联会导致RAG-1和RAG-2基因表达快速、特异性且可逆地下调。我们还发现,一小部分但比例显著的正常带有表面免疫球蛋白的骨髓B细胞表达RAG-1基因。在从前B细胞到B细胞转变过程中对特定基因表达控制的可能影响的背景下讨论了这些发现。
