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首页> 外文期刊>Journal of cell biology >Mammalian p55CDC Mediates Association of the Spindle Checkpoint Protein Mad2 with the Cyclosome/Anaphase-promoting Complex, and is Involved in Regulating Anaphase Onset and Late Mitotic Events
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Mammalian p55CDC Mediates Association of the Spindle Checkpoint Protein Mad2 with the Cyclosome/Anaphase-promoting Complex, and is Involved in Regulating Anaphase Onset and Late Mitotic Events

机译:哺乳动物p55CDC介导纺锤体检查点蛋白Mad2与环体/后期促进复合体的关联,并参与调节后期发作和晚期有丝分裂事件。

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We have investigated the function of p55CDC, a mammalian protein related to Cdc20 and Hct1/Cdh1 in Saccharomyces cerevisiae , and Fizzy and Fizzy-related in Drosophila . Immunofluorescence studies and expression of a p55CDC-GFP chimera demonstrate that p55CDC is concentrated at the kinetochores in M phase cells from late prophase to telophase. Some p55CDC is also associated with the spindle microtubules and spindle poles, and some is diffuse in the cytoplasm. At anaphase, the concentration of p55CDC at the kinetochores gradually diminishes, and is gone by late telophase. In extracts prepared from M phase, but not from interphase HeLa cells, p55CDC coimmunoprecipitates with three important elements of the M phase checkpoint machinery: Cdc27, Cdc16, and Mad2. p55CDC is required for binding Mad2 with the Cdc27 and Cdc16. Thus, it is likely that p55CDC mediates the association of Mad2 with the cyclosome/anaphase-promoting complex. Microinjection of anti-p55CDC antibody into mitotic mammalian cells induces arrest or delay at metaphase, and impairs progression of late mitotic events. These studies suggest that mammalian p55CDC may be part of a regulatory and targeting complex for the anaphase-promoting complex.
机译:我们已经研究了p55CDC的功能,p55CDC是在酿酒酵母中与Cdc20和Hct1 / Cdh1相关的蛋白,在果蝇中与Fizzy和Fizzy相关。免疫荧光研究和p55CDC-GFP嵌合体的表达表明,p55CDC从前期晚期到末期都集中在M期细胞的动粒体中。一些p55CDC也与纺锤体微管和纺锤体极相关,而一些则在细胞质中扩散。在后期,动植物体内p55CDC的浓度逐渐降低,并在末期逐渐消失。在从M期而不是从相间HeLa细胞制备的提取物中,p55CDC与M期关卡机制的三个重要元素共同免疫沉淀:Cdc27,Cdc16和Mad2。将Mad2与Cdc27和Cdc16绑定需要p55CDC。因此,p55CDC可能介导了Mad2与环体/后期促进复合物的缔合。将抗p55CDC抗体显微注射到有丝分裂的哺乳动物细胞中会诱导中期的停滞或延迟,并损害晚期有丝分裂事件的进程。这些研究表明,哺乳动物p55CDC可能是后期促进复合物的调控和靶向复合物的一部分。

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