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肠细胞Caco-2细胞对葡萄糖的适应性通过将三酰甘油靶向内质网腔来调节富含三酰甘油的脂蛋白分泌。

Adaptation of enterocytic Caco-2 cells to glucose modulates triacylglycerol-rich lipoprotein secretion through triacylglycerol targeting into the endoplasmic reticulum lumen.

作者信息

Pauquai Thomas, Bouchoux Julien, Chateau Danielle, Vidal Romain, Rousset Monique, Chambaz Jean, Demignot Sylvie

机构信息

UMR 505 INSERM-Université Pierre et Marie Curie and Laboratoire de Pharmacologie Cellulaire de l'Ecole Pratique des Hautes Etudes, Centre de Recherches Biomédicales des Cordeliers, 15 rue de l'Ecole de Médecine, 75006 Paris, France.

出版信息

Biochem J. 2006 Apr 15;395(2):393-403. doi: 10.1042/BJ20051359.

Abstract

Enterocytes are responsible for the absorption of dietary lipids, which involves TRL [TG (triacylglycerol)-rich lipoprotein] assembly and secretion. In the present study, we analysed the effect on TRL secretion of Caco-2 enterocyte adaptation to a differential glucose supply. We showed that TG secretion in cells adapted to a low glucose supply for 2 weeks after confluence was double that of control cells maintained in high-glucose-containing medium, whereas the level of TG synthesis remained similar in both conditions. This increased secretion resulted mainly from an enlargement of the mean size of the secreted TRL. The increased TG availability for TRL assembly and secretion was not due to an increase in the MTP (microsomal TG transfer protein) activity that is required for lipid droplet biogenesis in the ER (endoplasmic reticulum) lumen, or to the channelling of absorbed fatty acids towards the monoacylglycerol pathway for TG synthesis. Interestingly, by electron microscopy and subcellular fractionation studies, we observed, in the low glucose condition, an increase in the TG content available for lipoprotein assembly in the ER lumen, with the cytosolic/microsomal TG levels being verapamil-sensitive. Overall, we demonstrate that Caco-2 enterocytes modulate TRL secretion through TG partitioning between the cytosol and the ER lumen according to the glucose supply. Our model will help in identifying the proteins involved in the control of the balance between TRL assembly and cytosolic lipid storage. This mechanism may be a way for enterocytes to regulate TRL secretion after a meal, and thus impact on our understanding of post-prandial hypertriglyceridaemia.

摘要

肠上皮细胞负责膳食脂质的吸收,这涉及富含甘油三酯(TG)的脂蛋白(TRL)的组装和分泌。在本研究中,我们分析了Caco-2肠上皮细胞适应不同葡萄糖供应对TRL分泌的影响。我们发现,汇合后适应低葡萄糖供应2周的细胞中TG分泌量是维持在含高葡萄糖培养基中的对照细胞的两倍,而两种条件下TG合成水平保持相似。这种分泌增加主要是由于分泌的TRL平均大小增大所致。TRL组装和分泌中TG可用性的增加并非由于内质网(ER)腔中脂滴生物合成所需的微粒体TG转移蛋白(MTP)活性增加,也不是由于吸收的脂肪酸向用于TG合成的单酰甘油途径的分流。有趣的是,通过电子显微镜和亚细胞分级分离研究,我们观察到在低葡萄糖条件下,ER腔中可用于脂蛋白组装的TG含量增加,胞质/微粒体TG水平对维拉帕米敏感。总体而言,我们证明Caco-2肠上皮细胞根据葡萄糖供应通过TG在胞质和ER腔之间的分配来调节TRL分泌。我们的模型将有助于确定参与控制TRL组装和胞质脂质储存之间平衡的蛋白质。这种机制可能是肠上皮细胞在餐后调节TRL分泌的一种方式,从而影响我们对餐后高甘油三酯血症的理解。

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