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CTTNBP2, but not CTTNBP2NL, regulates dendritic spinogenesis and synaptic distribution of the striatin–PP2A complex

机译:CTTNBP2,而不是CTTNBP2NL,调节striatin-PP2A复合物的树突棘发生和突触分布

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Cortactin-binding protein 2 (CTTNBP2) interacts with cortactin to regulate cortactin mobility and control dendritic spine formation. CTTNBP2 has also been associated with autistic spectrum disorder. The regulation of dendritic spinogenesis could explain the association of CTTNBP2 with autism. Sequence comparison has indicated that CTTNBP2 N-terminal–like protein (CTTNBP2NL) is a CTTNBP2 homologue. To confirm the specific effect of CTTNBP2 on dendritic spinogenesis, here we investigate whether CTTNBP2NL has a similar function to CTTNBP2. Although both CTTNBP2 and CTTNBP2NL interact with cortactin, CTTNBP2NL is associated with stress fibers, whereas CTTNBP2 is distributed to the cortex and intracellular puncta. We also provide evidence that CTTNBP2, but not CTTNBP2NL, is predominantly expressed in the brain. CTTNBP2NL does not show any activity in the regulation of dendritic spinogenesis. In addition to spine morphology, CTTNBP2 is also found to regulate the synaptic distribution of striatin and zinedin (the regulatory B subunits of protein phosphatase 2A [PP2A]), which interact with CTTNBP2NL in HEK293 cells. The association between CTTNBP2 and striatin/zinedin suggests that CTTNBP2 targets the PP2A complex to dendritic spines. Thus we propose that the interactions of CTTNBP2 and cortactin and the PP2A complex regulate spine morphogenesis and synaptic signaling.
机译:Cortactin结合蛋白2(CTTNBP2)与cortactin相互作用,以调节cortactin的活动性并控制树突状脊柱的形成。 CTTNBP2也与自闭症谱系障碍有关。树突状棘发生的调节可以解释CTTNBP2与自闭症的关系。序列比较表明CTTNBP2 N末端样蛋白(CTTNBP2NL)是CTTNBP2的同源物。为了确认CTTNBP2对树突状棘发生的特定作用,在这里我们调查CTTNBP2NL是否具有与CTTNBP2类似的功能。尽管CTTNBP2和CTTNBP2NL均与皮质激素相互作用,但CTTNBP2NL与应力纤维相关,而CTTNBP2则分布于皮质和细胞内点。我们还提供了CTTNBP2而不是CTTNBP2NL在大脑中主要表达的证据。 CTTNBP2NL在调节树突棘发生中没有任何活性。除了脊柱形态外,还发现CTTNBP2调节striatin和zinedin(蛋白磷酸酶2A [PP2A]的调节B亚基)的突触分布,它们在HEK293细胞中与CTTNBP2NL相互作用。 CTTNBP2和striatin / zinedin之间的关联表明,CTTNBP2将PP2A复合物靶向树突棘。因此,我们建议CTTNBP2和cortactin和PP2A复杂的相互作用调节脊柱形态发生和突触信号。

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