首页> 外文期刊>Molecular and Cellular Biochemistry: An International Journal for Chemical Biology >Lysophosphatidic acid, alkylglycerophosphate and alkylacetylglycerophosphate increase the neuronal nuclear acetylation of 1-acyl lysophosphatidyl choline by inhibition of lysophospholipase.
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Lysophosphatidic acid, alkylglycerophosphate and alkylacetylglycerophosphate increase the neuronal nuclear acetylation of 1-acyl lysophosphatidyl choline by inhibition of lysophospholipase.

机译:溶血磷脂酸,烷基甘油磷酸酯和烷基乙酰基甘油磷酸酯通过抑制溶血磷脂酶增加了1-酰基溶血磷脂酰胆碱的神经元核乙酰化。

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摘要

Neuronal nuclei were isolated from rabbit cerebral cortex, and lipid acetylation reactions were studied because of the high nuclear concentration of acetyltransferases that generate platelet activating factor (PAF) and its acyl analogue AcylPAF. The neuronal nuclear acetylation of 1-palmitoyl lysophosphatidylcholine (lyso PC) was found to be increased more than twofold when low concentrations of lyso PC were incubated in acetylation assays in the presence of 1-palmitoyl lysophosphatidic acid (lyso PA) or 1-hexadecyl glycerophosphate (AGP). This effect was not found for a variety of other acidic and neutral 1-acyl lysoglycerophospholipids. At 4 microM concentrations, AGP was the more effective in increasing rates of lyso PC acetylation, while lyso PA was more effective at 25-35 microM. 1-Stearoyl, 1-alkenyl and 1-decanoyl analogues of lyso PA were all less effective than 1-palmitoyl lyso PA. Phosphatidic acid was considerably less effective than lyso PA, while the acetylated analogue of AGP, AAcGP (alkylacetylglycerophosphate), increased rates of lyso PC acetylation to maxima similar to those seen with lyso PA or AGP. In addition, AAcGP promoted these maxima at considerably lower concentrations (2-4 microM). A mechanism for these effects was suggested when nuclear envelopes (NE), isolated in the presence of PMSF, showed these maximal acetylation rates at low lyso PC concentrations, and these rates were not elevated by the presence of lyso PA. PMSF is a protease inhibitor but can also inhibit lysophospholipase activity. We found a nuclear lysophospholipase that degraded lyso PC at rates more than 13 times those of nuclear lyso PC acetylation. PMSF did inhibit this nuclear lysophospholipase, as did lyso PA, AGP and AAcGP. Kinetic analyses of the effects of lyso PA, AGP and AAcGP on lyso PC lysophospholipase indicated that these three lipids acted as competitive inhibitors for the lyso PC substrate. It is possible that low rates of lyso PC acetylation seen in neuronal nuclei at low lyso PC concentrations, are caused by lyso PC loss mediated by a very strong nuclear lysophospholipase. The effects of lyso PA, AGP and AAcGP in boosting rates of lyso PC acetylation likely come from the inhibition of nuclear lysophospholipase and a preservation of lyso PC concentrations. Competing neuronal nuclear reactions for low endogenous levels of lyso PC may regulate the formation of AcylPAF, and rising lyso PA, AGP or AAcGP concentrations can increase rates of nuclear AcylPAF synthesis.
机译:从兔大脑皮层中分离出神经元核,并研究了脂质乙酰化反应,因为乙酰核转移酶的高核浓度会产生血小板活化因子(PAF)及其酰基类似物AcylPAF。当在1-棕榈酰基溶血磷脂酸(lyso PA)或1-十六烷基甘油磷酸酯存在下进行乙酰化试验时,将低浓度的lyso PC在乙酰化反应中孵育时,发现1-棕榈酰基溶血磷脂酰胆碱(lyso PC)的神经元核乙酰化增加了两倍以上。 (AGP)。对于多种其他酸性和中性的1-酰基溶血甘油磷脂未发现这种作用。在4 microM浓度下,AGP在提高溶血PC乙酰化率方面更有效,而溶血PA在25-35 microM时更有效。溶血素PA的1-硬脂酰基,1-烯基和1-癸酰基类似物均不如1-棕榈酰基溶血素PA有效。磷脂酸的功效远不如溶血PA,而AGP的乙酰化类似物AAcGP(烷基乙酰基甘油磷酸)使溶血PC乙酰化的速率增加到最大值,与溶血PA或AGP相似。此外,AAcGP以较低的浓度(2-4 microM)促进了这些最大值。当在PMSF存在下分离的核被膜(NE)在低溶血素PC浓度下显示出最大的乙酰化速率,而溶血素PA的存在并未提高这些速率时,则提示了这些作用的机制。 PMSF是蛋白酶抑制剂,但也可以抑制溶血磷脂酶活性。我们发现了一种核溶血磷脂酶,其降解溶血PC的速率是核溶血PC乙酰化的13倍以上。 PMSF确实能抑制这种核溶血磷脂酶,而溶血PA,AGP和AAcGP也是如此。动力学分析溶血PA,AGP和AAcGP对溶血PC溶血磷脂酶的影响表明,这三种脂质充当溶血PC底物的竞争性抑制剂。在低溶血素PC浓度下在神经元核中观察到的溶血素PC乙酰化率低可能是由非常强的核溶血磷脂酶介导的溶血素PC损失引起的。溶血PA,AGP和AAcGP对溶血PC乙酰化速率的提高可能来自抑制核溶血磷脂酶和保持溶血PC浓度。低内源性溶血素PC的竞争性神经核反应可能会调节AcylPAF的形成,而溶血PA,AGP或AAcGP浓度的升高会增加核AcylPAF的合成速率。

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