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Dual function of the NDR-kinase Dbf2 in the regulation of the F-BAR protein Hof1 during cytokinesis

机译:NDR激酶Dbf2在胞质分裂过程中调控F-BAR蛋白Hof1的双重功能

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摘要

The conserved NDR-kinase Dbf2 plays a critical role in cytokinesis in budding yeast. Among its cytokinesis-related substrates is the F-BAR protein Hof1. Hof1 colocalizes at the cell division site with the septin complex and, as mitotic exit progresses, moves to the actomyosin ring (AMR). Neither the function of Hof1 at the septin complex nor the mechanism by which Hof1 supports AMR constriction is understood. Here we establish that Dbf2 has a dual function in Hof1 regulation. First, we show that the coiled-coil region, which is adjacent to the conserved F-BAR domain, is required for the binding of Hof1 to septins. The Dbf2-dependent phosphorylation of Hof1 at a single serine residue (serine 313) in this region diminishes the recruitment of Hof1 to septins both in vitro and in vivo. Genetic and functional analysis indicates that the binding of Hof1 to septins is important for septin rearrangement and integrity during cytokinesis. Furthermore, Dbf2 phosphorylation of Hof1 at serines 533 and 563 promotes AMR constriction most likely by inhibiting the SH3-domain–dependent interactions of Hof1. Thus our data show that Dbf2 coordinates septin and AMR functions during cytokinesis through the regulation/control of Hof1.
机译:保守的NDR激酶Dbf2在发芽酵母的胞质分裂中起关键作用。 F-BAR蛋白Hof1是其胞质分裂相关底物之一。 Hof1与septin复合物共定位在细胞分裂部位,并且随着有丝分裂出口的进展,移至放线菌素环(AMR)。既不了解Hof1在Septin复合体上的功能,也不了解Hof1支持AMR收缩的机制。在这里,我们确定Dbf2在Hof1调节中具有双重功能。首先,我们显示Hof1与septins的结合需要与保守的F-BAR域相邻的卷曲螺旋区域。 Hof1在此区域中的单个丝氨酸残基(丝氨酸313)的Dbf2依赖性磷酸化减少了Hof1在体内和体外的募集。遗传和功能分析表明,Hof1与Septins的结合对于在胞质分裂过程中Septin重排和完整性很重要。此外,丝氨酸533和563处Hof1的Dbf2磷酸化最有可能通过抑制Hof1的SH3结构域依赖性相互作用来促进AMR收缩。因此,我们的数据表明,Dbf2通过Hof1的调控来协调细胞分裂过程中的septin和AMR功能。

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