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DGK and nuclear signaling nuclear diacylglycerol kinases in IIC9 cells

机译:DGK和核信号核信号核二酰基甘油激酶在IIC9细胞中

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Our investigations of DGK in IIC9 nuclei revealed the presence of two isoforms: DGK θ, which is regulated upon stimulation with the growth factor α-thrombin, and DGK δ, which is constitutively active during the investigated time course. We have previously determined that following α-thrombin stimulation, RhoA translocates to the nucleus and activates a PC-PLD1 activity. Our data indicate that RhoA inhibits nuclear DGKθ activity, suggesting that RhoA acts as a regulator to switch PA production from DGK to PC-PLD. We further suggest that the species profile of PA resulting from the two enzyme activities is likely to be different, and that there may be a topological diversity to the two pools of PA. In addition, we have identified an α-thrombin-sensitive nuclear PI-PLC activity, and have further determined that DGK9 and the PI-PLC are both localized to the nuclear lysate fraction, suggesting that DGKθ may play a role in a nuclear PI cycle. Whether the DGKθ-produced PA is a nuclear second messenger, a precursor for nuclear PI, or both, remains an open question.
机译:我们在DGK细胞核IIC9的调查显示两种同种型的存在:DGKθ,这是在与生长因子α凝血酶刺激调节,DGKδ,其中所研究的时间过程中是组成性激活。我们先前已经决定,下列α凝血酶刺激,RhoA的转移到细胞核并激活PC-PLD1活动。我们的数据表明RhoA的抑制核DGKθ活动,这表明RhoA的行为作为监管机构从DGK切换PA生产,以PC-PLD。我们进一步认为,PA的从两个酶活动产生的物种外形很可能是不同的,这有可能是一个拓扑多样性PA的两个游泳池。此外,我们已经确定了α凝血酶敏感核PI-PLC的活性,并进一步确定,DGK9和PI-PLC均定位于核裂解分数,这表明DGKθ可以在核PI周期发挥作用。是否DGKθ产生的PA是核的第二信使,核PI前体,或两者,仍然是一个有待解决的问题。

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