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Phospholipase D-induced phosphatidate production in intact small arteries during noradrenaline stimulation: involvement of both G-protein and tyrosine-phosphorylation-linked pathways.

机译：去甲肾上腺素刺激过程中磷脂酶D诱导完整小动脉中的磷脂酸生成：G蛋白和酪氨酸磷酸化相关途径均参与。

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To investigate membrane lipid metabolism during smooth-muscle activation, the role of phospholipase D (PLD) in the production of phosphatidate (PA) was studied in rat small arteries stimulated with noradrenaline. Incubation with [3H]myristate preferentially labelled phosphatidylcholine (PtdCho), and in the presence of 0.5% ethanol [3H]phosphatidylethanol ([3H]PEt) was formed, demonstrating PLD activity. Noradrenaline (NA) stimulation resulted in an increase in PtdCho derived [3H]PA and [3H]PEt formation, indicating PLD activation. Stimulation of [14C]choline release confirmed PLD-mediated hydrolysis of PtdCho. Propranolol, an inhibitor of PA phosphohydrolase, increased [3H]PA levels in non-stimulated tissue and decreased the rate of degradation of both [3H]PA and [3H]PEt, implying that this is an active route for PA metabolism in small arteries. However, [3H]diacylglycerol levels were not increased during NA stimulation. Fluoroaluminate increased [3H]PEt formation and [14C]choline release, whereas high K+ in the presence of alpha 1-adrenoceptor blockade did not. Pervanadate increased phosphotyrosine levels in small arteries, and markedly stimulated [3H]PEt formation and [14C]choline release. The combination of pervanadate and NA stimulation resulted in a dramatic increase in [3H]PEt formation, which was greater than the sum of the individual responses to the two agonists. Pervanadate and fluoroaluminate in combination appeared to give an additive response, whereas high K+ did not alter the pervanadate-induced formation of [3H]PEt. Phosphotyrosine levels were increased by NA in the presence of tyrosine phosphatase inhibitors. This effect was blocked by genistein, a tyrosine kinase inhibitor. These data demonstrate that in NA-stimulated small arteries PLD-induced PtdCho hydrolysis contributes to accumulation of PA, but not of diacylglycerol. Furthermore, regulation of PLD activity appears to require G-protein and tyrosine-phosphorylation-linked pathways.

机译：为了研究平滑肌激活过程中的膜脂质代谢，在去甲肾上腺素刺激的大鼠小动脉中研究了磷脂酶D（PLD）在磷脂酸（PA）产生中的作用。与[3H]肉豆蔻酸酯优先标记的磷脂酰胆碱（PtdCho）一起孵育，并在存在0.5％乙醇的情况下，形成了[3H]磷脂酰乙醇（[3H] PEt），证明了PLD的活性。去甲肾上腺素（NA）刺激导致PtdCho衍生的[3H] PA和[3H] PEt形成增加，表明PLD激活。刺激[14C]胆碱释放证实了PLD介导的PtdCho水解。普萘洛尔，PA磷酸水解酶的抑制剂，在未刺激的组织中增加[3H] PA的水平，并降低[3H] PA和[3H] PEt的降解速率，这暗示这是小动脉中PA代谢的有效途径。然而，在NA刺激期间[3H]二酰甘油水平没有增加。氟铝酸盐增加了[3H] PEt的形成和[14C]胆碱的释放，而在存在α1-肾上腺素受体阻滞剂时，高K +却没有。过钒酸盐增加了小动脉中磷酸酪氨酸的水平，并显着刺激了[3H] PEt的形成和[14C]胆碱的释放。过钒酸盐和NA刺激的组合导致[3H] PEt形成的急剧增加，这大于对两种激动剂的个体反应的总和。过氧钒酸盐和氟铝酸盐的组合似乎会产生加和反应，而高K +不会改变过氧钒酸盐诱导的[3H] PEt的形成。在酪氨酸磷酸酶抑制剂的存在下，NA可提高磷酸酪氨酸水平。酪氨酸激酶抑制剂染料木黄酮可阻止这种作用。这些数据表明，在NA刺激的小动脉中，PLD诱导的PtdCho水解有助于PA的蓄积，而不是二酰基甘油的蓄积。此外，PLD活性的调节似乎需要G蛋白和酪氨酸磷酸化相关的途径。

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期刊名称 Biochemical Journal
作者
D T Ward; J Ohanian; A M Heagerty; V Ohanian;
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年(卷),期 1995(307),Pt 2
年度 1995
页码 451–456
总页数 6
原文格式 PDF
正文语种
中图分类分子生物学;
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专利

1. PHOSPHOLIPASE D-INDUCED PHOSPHATIDATE PRODUCTION IN INTACT SMALL ARTERIES DURING NORADRENALINE STIMULATION - INVOLVEMENT OF BOTH G-PROTEIN AND TYROSINE-PHOSPHORYLATION-LINKED PATHWAYS [J] . Ward DT, Ohanian J, Heagerty AM, The Biochemical Journal . 1995,第Pta2期

机译：去甲肾上腺素刺激过程中磷脂酶D诱导完整小动脉中的磷脂生产-G蛋白和酪氨酸磷酸化相关途径的参与
2. Phospholipase D-induced phosphatidate production in intact small arteries during noradrenaline stimulation: involvement of both G-protein and tyrosine-phosphorylation-linked pathways [J] . A M Heagerty, D T Ward, J Ohanian, The biochemical journal . 1995,第2期

机译：去甲肾上腺素刺激过程中磷脂酶D诱导的完整小动脉中磷脂酸的产生：G蛋白和酪氨酸磷酸化相关途径的参与
3. Stimulation of phosphatidate synthesis in endothelial cells in response to P2-receptor activation. Evidence for phospholipase C and phospholipase D involvement, phosphatidate and diacylglycerol interconversion and the role of protein kinase C [J] . J R Purkiss, M R Boarder The biochemical journal . 1992,第1期

机译：响应P2受体激活刺激内皮细胞中的磷脂酸酯合成。磷脂酶C和磷脂酶D参与，磷脂酸酯和二酰基甘油相互转化以及蛋白激酶C的作用的证据
4. INVOLVEMENT OF TGF- β IN INHIBITORY EFFECTS OF NEGATIVELY CHARGED LIPOSOMES ON NITRIC OXIDE PRODUCTION BY MACROPHAGES STIMULATED WITH LPS [C] . Y. Aramaki, R.Matsuno, S. Tsuchiya International symposium on controlled release of bioactive materials;Consumer diversified products conference . 2001

机译：负电荷脂质体对脂多糖刺激的巨噬细胞产生一氧化氮的抑制作用中TGF-β的参与
5. Vasoconstrictor-stimulated phosphoinositide signalling in caveolae/lipid rafts of intact small arteries [D] . Clarke, Christopher James. 2005

机译：血管收缩剂刺激的完整小动脉海绵体/脂质筏中的磷酸肌醇信号转导
6. Stimulation of phosphatidate synthesis in endothelial cells in response to P2-receptor activation. Evidence for phospholipase C and phospholipase D involvement phosphatidate and diacylglycerol interconversion and the role of protein kinase C. [O] . J R Purkiss, M R Boarder 1992

机译：响应P2受体激活刺激内皮细胞中的磷脂酸酯合成。磷脂酶C和磷脂酶D参与磷脂酸酯和二酰基甘油相互转化以及蛋白激酶C的作用的证据。
7. Phospholipase D-induced phosphatidate production in intact small arteries during noradrenaline stimulation: involvement of both G-protein and tyrosine-phosphorylation-linked pathways. [O] . Ward, D T, Ohanian, J, Heagerty, A M, 1995

机译：去甲肾上腺素刺激过程中磷脂酶D诱导完整小动脉中的磷脂酸生成：G蛋白和酪氨酸磷酸化相关途径均参与。

Phospholipase D-induced phosphatidate production in intact small arteries during noradrenaline stimulation: involvement of both G-protein and tyrosine-phosphorylation-linked pathways.

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