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靶向 UBXD8 和 AAM-B 的序列表明内质网在脂滴的出现和消退中具有直接作用。

Targeting sequences of UBXD8 and AAM-B reveal that the ER has a direct role in the emergence and regression of lipid droplets.

机构信息

Department of Cell Biology, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.

出版信息

J Cell Sci. 2009 Oct 15;122(Pt 20):3694-702. doi: 10.1242/jcs.054700. Epub 2009 Sep 22.

Abstract

Lipid droplets are sites of neutral lipid storage thought to be actively involved in lipid homeostasis. A popular model proposes that droplets are formed in the endoplasmic reticulum (ER) by a process that begins with the deposition of neutral lipids between the membrane bilayer. As the droplet grows, it becomes surrounded by a monolayer of phospholipid derived from the outer half of the ER membrane, which contains integral membrane proteins anchored by hydrophobic regions. This model predicts that for an integral droplet protein inserted into the outer half of the ER membrane to reach the forming droplet, it must migrate in the plane of the membrane to sites of lipid accumulation. Here, we report the results of experiments that directly test this hypothesis. Using two integral droplet proteins that contain unique hydrophobic targeting sequences (AAM-B and UBXD8), we present evidence that both proteins migrate from their site of insertion in the ER to droplets that are forming in response to fatty acid supplementation. Migration to droplets occurs even when further protein synthesis is inhibited or dominant-negative Sar1 blocks transport to the Golgi complex. Surprisingly, when droplets are induced to disappear from the cell, both proteins return to the ER as the level of neutral lipid declines. These data suggest that integral droplet proteins form from and regress to the ER as part of a cyclic process that does not involve traffic through the secretory pathway.

摘要

脂滴是中性脂质储存的场所,被认为积极参与脂质动态平衡。一个流行的模型提出,滴状物是在内质网(ER)中形成的,其过程始于在膜双层之间沉积中性脂质开始。随着液滴的生长,它被来自 ER 膜外半部分的单层磷脂包围,该膜含有由疏水区锚定的整合膜蛋白。该模型预测,对于插入 ER 膜外半部分的完整液滴蛋白要到达正在形成的液滴,它必须在膜平面内向脂质积累的部位迁移。在这里,我们报告了直接测试该假设的实验结果。使用含有独特疏水性靶向序列(AAM-B 和 UBXD8)的两种完整的液滴蛋白,我们提供的证据表明,这两种蛋白都从它们在 ER 中的插入部位迁移到响应脂肪酸补充而形成的液滴。即使进一步的蛋白质合成被抑制或显性负性 Sar1 阻断向高尔基体的运输,迁移到液滴也会发生。令人惊讶的是,当液滴被诱导从细胞中消失时,随着中性脂质水平的下降,两种蛋白都返回 ER。这些数据表明,整合的液滴蛋白作为一个不涉及分泌途径的循环过程的一部分从 ER 形成并回归 ER。

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