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首页> 外文期刊>Experimental parasitology >Entamoeba invadens: sphingolipids metabolic regulation is the main component of a PKC signaling pathway in controlling cell growth and proliferation.
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Entamoeba invadens: sphingolipids metabolic regulation is the main component of a PKC signaling pathway in controlling cell growth and proliferation.

机译:Entamoeba入侵:鞘脂的代谢调节是控制细胞生长和增殖的PKC信号通路的主要组成部分。

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摘要

The sphingolipids biosynthesis pathway generates bioactive molecules crucial to the regulation of physiological processes. We have recently reported that DAG (diacylglycerol) generated during sphingomyelin synthesis, plays an important role in PKC (protein kinase C) activation, necessary for the transit through the cell cycle (G1 to S transition) and cell proliferation (Cerbon and Lopez-Sanchez, 2003. Diacylglycerol generated during sphingomyelin synthesis is involved in protein kinase C activation and cell proliferation in Madin-Darby canine kidney cells. Biochem. J. 373, 917-924). Since pathogenic Entamoeba invadens synthesize the sphingolipids inositol-phosphate ceramide (IPC) and ethanolamine-phosphate ceramide (EPC) as well as sphingomyelin (SM), we decided to investigate when during growth initiation, the synthesis of sphingolipids takes place, DAG is generated and PKC is activated. We found that during the first 6 h of incubation there was a significant increase in the synthesis of all three sphingolipids, accompanied by a progressive increment (up to 4-fold) in the level of DAG, and particulate PKC activity was increased 4-8 times. The enhanced DAG levels coincided with decrements in the levels of sphingoid bases, conditions adequate for the activation of PKC. Moreover, we found that inhibition of sphingolipid synthesis with myriocin, specific inhibitor of the synthesis of sphinganine, reduce DAG generation, PKC activation and cell proliferation. All these inhibitory processes were restored by metabolic complementation with exogenous D-erythrosphingosine, indicating that the DAG generated during sphingolipid synthesis was necessary for PKC activation and cell proliferation. Also, we show that PI (phosphatidylinositol), PE (phosphatidylethanolamine) and PC (phosphatidylcholine) are the precursors of their respective sphingolipids (IPC, EPC and SM), and therefore sources of DAG to activate PKC.
机译:鞘脂生物合成途径产生对调节生理过程至关重要的生物活性分子。我们最近报道,在鞘磷脂合成过程中产生的DAG(甘油二酯)在PKC(蛋白激酶C)激活中起重要作用,这对于通过细胞周期(从G1到S的过渡)和细胞增殖(Cerbon和Lopez-Sanchez)是必不可少的,鞘磷脂合成期间产生的二酰基甘油参与Madin-Darby犬肾细胞中的蛋白激酶C活化和细胞增殖(Biochem.J.373,917-924)。由于致病性 Entamoeba入侵合成了鞘脂肌醇-磷酸神经酰胺(IPC)和乙醇胺-磷酸神经酰胺(EPC)以及鞘磷脂(SM),因此我们决定研究在生长开始时什么时候鞘脂的合成发生时,将生成DAG并激活PKC。我们发现,在孵育的前6小时内,所有三种鞘脂的合成均显着增加,同时DAG的水平逐渐增加(最多4倍),并且颗粒PKC活性提高了4-8次。 DAG水平的增加与鞘氨醇碱水平的下降相吻合,这是激活PKC的条件。此外,我们发现用鼠尾草素(鞘氨醇合成的特异性抑制剂)抑制鞘脂合成可减少DAG生成,PKC活化和细胞增殖。所有这些抑制过程都通过与外源D-赤藓红神经鞘糖的代谢互补而得以恢复,这表明鞘脂合成过程中产生的DAG对于PKC活化和细胞增殖是必需的。此外,我们显示PI(磷脂酰肌醇),PE(磷脂酰乙醇胺)和PC(磷脂酰胆碱)是它们各自的鞘脂(IPC,EPC和SM)的前体,因此是DAG激活PKC的来源。

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