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首页> 外文期刊>Biochimica et Biophysica Acta. Molecular and cell biology of Lipids >13C-labelling studies indicate compartmentalized synthesis of triacylglycerols in C6 rat glioma cells.
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13C-labelling studies indicate compartmentalized synthesis of triacylglycerols in C6 rat glioma cells.

机译:13C标记研究表明在C6大鼠神经胶质瘤细胞中三酰基甘油的区室合成。

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摘要

NMR-visible mobile lipid (ML) signals have been detected in (1)H-NMR spectra of tissues in vivo, ex vivo and in vitro, and have been shown to change in apparent intensity in association with pathology (necrosis in brain tumours) and normal processes (cell differentiation, cell growth arrest and apoptosis). Although it is widely accepted that ML signals originate mainly from fatty-acyl chains in triacylglycerols (TAG) contained in cytosolic lipid droplets (LD), the dynamics of TAG in LD is not yet fully understood. In order to better understand the synthesis of cellular TAG and its relationship to ML dynamics we carried out a set of labelling experiments with C6 rat glioma cells in culture. TAG and phospholipid metabolism was monitored by incubating C6 cells with [1-(13)C]-glucose at two time points during cell growth curve -24 h incubation starting at log-phase; 48 h incubation starting at saturation density- and by acquiring the 2D-HMQC NMR spectra of the respective total lipid extracts. The resulting TAG, diacylglycerol (DAG) and phospholipid labelling patterns can only be explained if TAG synthesis takes place in two different subcellular compartments. One compartment would be the endoplasmic reticulum, which is known to be involved in TAG metabolism, while the other compartment could be the plasma membrane and/or the LD. This possible role of LD is further supported by the recent description of diacylglycerolacyltranferase-activity associated with LD. Accordingly, we postulate the existence of a carbon-shuttling mechanism between plasma membrane phospholipids and endoplasmic reticulum by way of LD content. The results we have obtained with C6 cells may also apply to other cellular systems and should be taken into account when interpreting ML dynamics detected by NMR in vivo.
机译:已在体内,离体和体外组织的(1)H-NMR光谱中检测到NMR可见的移动脂质(ML)信号,并已显示出与病理学(脑肿瘤坏死)相关的表观强度变化和正常过程(细胞分化,细胞生长停滞和凋亡)。尽管人们普遍认为ML信号主要来源于胞浆脂质小滴(LD)中所含的三酰甘油(TAG)中的脂肪酰基链,但尚未完全了解LD中TAG的动力学。为了更好地了解细胞TAG的合成及其与ML动力学的关系,我们对培养的C6大鼠神经胶质瘤细胞进行了一系列标记实验。通过在对数期开始的细胞生长曲线-24 h的培养过程中的两个时间点,将C6细胞与[1-(13)C]葡萄糖一起培养,从而监控TAG和磷脂代谢。从饱和密度开始并通过获取各个总脂质提取物的2D-HMQC NMR光谱开始孵育48小时。仅当TAG合成发生在两个不同的亚细胞区室中时,才能解释得到的TAG,二酰基甘油(DAG)和磷脂标记模式。一个隔室是内质网,已知参与TAG代谢,而另一个隔室可以是质膜和/或LD。 LD的这种可能的作用由与LD有关的二酰基甘油糖基乳糖基转移酶活性的最新描述进一步支持。因此,我们通过LD含量推测质膜磷脂与内质网之间存在碳穿梭机制。我们用C6细胞获得的结果也可能适用于其他细胞系统,并且在解释通过NMR在体内检测到的ML动力学时应予以考虑。

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