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Protein kinase C regulates the nuclear localization of diacylglycerol kinase-zeta (see comments)

机译:蛋白激酶C调节二酰基甘油激酶-zeta的核定位(请参阅评论)

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Diacylglycerol kinases (DGKs) terminate signalling from diacylglycerol by converting it to phosphatidic acid. Diacylglycerol regulates cell growth and differentiation, and its transient accumulation in the nucleus may be particularly important in this regulation. Here we show that a fraction of DGK-zeta is found in the nucleus, where it regulates the amount of nuclear diacylglycerol. Reducing nuclear diacylglycerol levels by conditional expression of DGK-zeta attenuates cell growth. The nuclear-localization signal of DGK-zeta is located in a region that is homologous to the phosphorylation-site domain of the MARCKS protein. This is, to our knowledge, the first evidence that this domain, which is a major target for protein kinase C, can localize a protein to the nucleus. Two isoforms of protein kinase C, but not others, regulate the localization of DGK-zeta. Our results define a cycle in which diacylglycerol activates protein kinase C, which then regulates the metabolism of diacylglycerol by alternating the intracellular location of DGK-zeta. This may be a general mechanism to control mitogenic signals that depend on nuclear diacylglycerol.
机译:二酰基甘油激酶(DGK)通过将二酰基甘油转化为磷脂酸来终止其信号传导。二酰基甘油调节细胞的生长和分化,其在细胞核中的短暂积累在这种调节中可能特别重要。在这里,我们显示在细胞核中发现了一部分DGK-zeta,它调节了核二酰基甘油的含量。通过DGK-zeta的条件表达降低核二酰基甘油水平可减弱细胞生长。 DGK-zeta的核定位信号位于与MARCKS蛋白的磷酸化位点域同源的区域。据我们所知,这是蛋白质激酶C的主要靶标这一结构域可以将蛋白质定位于细胞核的第一个证据。蛋白激酶C的两个同工型,但不其他,调节DGK-zeta的定位。我们的结果定义了一个周期,其中二酰基甘油激活蛋白激酶C,然后通过交替改变DGK-zeta的细胞内位置来调节二酰基甘油的代谢。这可能是控制依赖核二酰基甘油的促有丝分裂信号的一般机制。

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