MgATP has different inhibitory effects on the use of 1-acyl-lysophosphatidylcholine and lyso platelet-activating factor acceptors by neuronal nuclear acetyltransferase activities

R.Roy Baker, Huu-yi Chang
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引用次数: 10

Abstract

The inhibitory effects of MgATP on neuronal nuclear acetyltransferase activities were studied using lyso platelet-activating factor (lyso-PAF, 1-alkyl-sn-glycero-3-phosphocholine) and lysophosphatidylcholine (lyso-PC, 1-acyl-sn-glycero-3-phosphocholine). The nuclear (N1) acetylation of lyso-PC was more profoundly inhibited by MgATP. MgATP did not alter the apparent Km for acetyl-CoA in either acetylation reaction. The inhibitory effects of MgATP were not seen for other nucleotides or MgAMP-PCP. Kinase inhibitors such as staurosporine (1 μM), chelerythrine, and R59022 (diglyceride kinase inhibitor I) did not block the MgATP inhibition of either acetylation. However, the addition of phospholipids to the assays indicated a selective inhibitory effect for PIP (25–50 μM) in the nuclear acetylation of lyso-PAF. When N1 was incubated with [γ-33P]ATP, phosphatidic acid and PIP were the principal radioactive lipid products. While the extent of MgATP inhibition of lyso-PAF acetylation was similar at different concentrations of lyso-PAF, increasing lyso-PC concentrations greatly decreased the MgATP inhibition seen in lyso-PC acetylations. Nuclear envelopes prepared in the presence of PMSF, and fraction N1 exposed to PMSF, did not show the inhibitory effect of MgATP on lyso-PC acetylation. PMSF (an inhibitor of certain phospholipase and lysophospholipase activities) did not reduce the MgATP inhibition of lyso-PAF acetylation. Arachidonoyl trifluoromethylketone, an inhibitor of cytosolic phospholipases A2 and of lysophospholipase activity associated with cPLA2, also blocked the inhibitory effect of MgATP on lyso-PC acetylation. Using radioactive lyso-PC substrate, fraction N1 produced labeled free fatty acid and phosphatidylcholine. In the presence of acetyl-CoA, the production of radioactive phosphatidylcholine increased almost 6-fold when MgATP was also included in these incubations. In the presence of MgATP and acetyl-CoA, PMSF reduced the levels of radioactive free fatty acid and phosphatidylcholine derived from lyso-PC, while Triacsin C, an inhibitor of acyl CoA synthetase, decreased phosphatidylcholine labeling. These findings suggest that MgATP inhibition of lyso-PC acetylation results from a loss of lyso-PC substrate that is largely mediated by nuclear lysophospholipase, acyl-CoA synthetase and lyso-PC acylation. Thus the neuronal nuclear production of Acyl PAF may be regulated by paths that compete for the lyso-PC substrate. In contrast, the acetylation of lyso-PAF is inhibited by PIP, a product of nuclear PI kinase reactions.

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MgATP通过神经元核乙酰转移酶活性对1-酰基溶血磷脂酰胆碱和溶酶血小板活化因子受体的使用有不同程度的抑制作用
采用溶血血小板活化因子(lyso- paf, 1-烷基-sn-甘油-3-磷酸胆碱)和溶血磷脂酰胆碱(lyso- pc, 1-酰基-sn-甘油-3-磷酸胆碱)研究MgATP对神经元核乙酰转移酶活性的抑制作用。MgATP对lyso-PC核(N1)乙酰化的抑制作用更明显。在两种乙酰化反应中,MgATP均未改变乙酰辅酶a的表观Km。mgamp对其他核苷酸或MgAMP-PCP的抑制作用未见。激酶抑制剂如staurosporine (1 μM), chelerythrine和R59022(双甘油酯激酶抑制剂I)不能阻断MgATP对乙酰化的抑制。然而,在实验中加入磷脂表明,PIP (25-50 μM)对lyso-PAF的核乙酰化有选择性抑制作用。当N1与[γ-33P]ATP孵育时,磷脂酸和PIP是主要的放射性脂质产物。虽然不同浓度的lyso-PAF对MgATP对lyso-PAF乙酰化的抑制程度相似,但增加lyso-PC浓度大大降低了MgATP对lyso-PC乙酰化的抑制作用。在PMSF存在下制备的核包膜和暴露于PMSF的N1片段均未显示MgATP对溶索- pc乙酰化的抑制作用。PMSF(某些磷脂酶和溶血磷脂酶活性的抑制剂)没有降低MgATP对溶血酶乙酰化的抑制作用。花生四烯酮三氟甲基酮是胞质磷脂酶A2和与cPLA2相关的溶血磷脂酶活性的抑制剂,也阻断了MgATP对溶血酶- pc乙酰化的抑制作用。利用放射性lyso-PC底物,N1馏分产生标记的游离脂肪酸和磷脂酰胆碱。在乙酰辅酶a存在的情况下,当MgATP也包含在这些孵育中时,放射性磷脂酰胆碱的产量增加了近6倍。在MgATP和乙酰辅酶a存在的情况下,PMSF降低了lyso-PC衍生的放射性游离脂肪酸和磷脂酰胆碱的水平,而酰基辅酶a合成酶抑制剂Triacsin C降低了磷脂酰胆碱的标记。这些发现表明,MgATP抑制溶索- pc乙酰化是由于溶索- pc底物的损失,这主要是由核溶磷脂酶、酰基辅酶a合成酶和溶索- pc酰化介导的。因此,神经元核酰基PAF的产生可能通过竞争溶酶- pc底物的途径来调节。相反,lyso-PAF的乙酰化被核PI激酶反应的产物PIP抑制。
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