首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Cell cycle-related shifts in subcellular localization of BCR: association with mitotic chromosomes and with heterochromatin.
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Cell cycle-related shifts in subcellular localization of BCR: association with mitotic chromosomes and with heterochromatin.

机译:BCR的亚细胞定位中与细胞周期相关的转变:与有丝分裂染色体和异染色质相关。

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摘要

The disruption of the BCR gene and its juxtaposition to and consequent activation of the ABL gene has been implicated as the critical molecular defect in Philadelphia chromosome-positive leukemias. The normal BCR protein is a multifunctional molecule with domains that suggest its participation in phosphokinase and GTP-binding pathways. Taken together with its localization to the cytoplasm of uncycled cells, it is therefore presumed to be involved in cytoplasmic signaling. By performing a double aphidicolin block for cell cycle synchronization, we currently demonstrate that the subcellular localization of BCR shifts from being largely cytoplasmic in interphase cells to being predominantly perichromosomal in mitosis. Furthermore, with the use of immunogold labeling and electron microscopy, association of BCR with DNA, in particular heterochromatin, can be demonstrated even in quiescent cells. Results were similar in cell lines of lymphoid or myeloid origin. These observations suggest a role for BCR in the phosphokinase interactions linked to condensed chromatin, a network previously implicated in cell cycle regulation.
机译:在费城染色体阳性白血病中,BCR基因的破坏及其与ABL基因的并置以及随之而来的活化被认为是关键的分子缺陷。正常的BCR蛋白是一种多功能分子,其结构域表明其参与了磷酸激酶和GTP结合途径。因此,连同其定位于未循环细胞的细胞质一起,它被认为参与了细胞质信号传导。通过执行双重aphidicolin块的细胞周期同步,我们目前证明BCR的亚细胞定位从相间细胞中的大部分细胞质转移到有丝分裂中的主要染色体周围。此外,通过使用免疫金标记和电子显微镜,甚至在静止细胞中也可以证明BCR与DNA的结合,特别是异染色质。淋巴或骨髓来源的细胞系的结果相似。这些发现表明BCR在与浓缩染色质相关的磷酸激酶相互作用中发挥了作用,该染色质先前与细胞周期调控有关。

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