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当前乳脂滴分泌机制模型的检验。

A test of current models for the mechanism of milk-lipid droplet secretion.

机构信息

Department of Animal and Avian Sciences, University of Maryland, College Park, MD 20742, USA.

出版信息

Traffic. 2013 Sep;14(9):974-86. doi: 10.1111/tra.12087. Epub 2013 Jun 23.

Abstract

Milk lipid is secreted by a unique process, during which triacylglycerol droplets bud from mammary cells coated with an outer bilayer of apical membrane. In all current schemes, the integral protein butyrophilin 1A1 (BTN) is postulated to serve as a transmembrane scaffold, which interacts either with itself or with the peripheral proteins, xanthine oxidoreductase (XOR) and possibly perilipin-2 (PLIN2), to form an immobile bridging complex between the droplet and apical surface. In one such scheme, BTN on the surface of cytoplasmic lipid droplets interacts directly with BTN in the apical membrane without binding to either XOR or PLIN2. We tested these models using both biochemical and morphological approaches. BTN was concentrated in the apical membrane in all species examined and contained mature N-linked glycans. We found no evidence for the association of unprocessed BTN with intracellular lipid droplets. BTN-enhanced green fluorescent protein was highly mobile in areas of mouse milk-lipid droplets that had not undergone post-secretion changes, and endogenous mouse BTN comprised only 0.5-0.7% (w/w) of the total protein, i.e. over 50-fold less than in the milk-lipid droplets of cow and other species. These data are incompatible with models of milk-lipid secretion in which BTN is the major component of an immobile global adhesive complex and suggest that interactions between BTN and other proteins at the time of secretion are more transient than previously predicted. The high mobility of BTN in lipid droplets marks it as a potential mobile signaling molecule in milk.

摘要

乳脂是通过一种独特的过程分泌的,在此过程中,三酰基甘油滴从覆盖有顶端膜外层双层的乳腺细胞中萌芽。在所有现行方案中,假定整合蛋白丁酸蛋白 1A1(BTN)充当跨膜支架,该支架与自身或与外周蛋白黄嘌呤氧化还原酶(XOR)和可能的 perilipin-2(PLIN2)相互作用,在液滴和顶端表面之间形成固定的桥接复合物。在这样的方案中,细胞质脂滴表面上的 BTN 与顶端膜中的 BTN 直接相互作用,而不与 XOR 或 PLIN2 结合。我们使用生化和形态学方法测试了这些模型。在检查的所有物种中,BTN 都集中在顶端膜中,并含有成熟的 N-连接糖基。我们没有发现未加工的 BTN 与细胞内脂滴之间存在关联的证据。BTN 增强型绿色荧光蛋白在未经历分泌后变化的小鼠乳脂滴区域中具有高度的流动性,而内源性小鼠 BTN 仅占总蛋白的 0.5-0.7%(w/w),即比牛和其他物种的乳脂滴中的含量低 50 多倍。这些数据与 BTN 是固定全局粘合复合物的主要成分的乳脂分泌模型不兼容,并表明 BTN 与分泌时其他蛋白质之间的相互作用比以前预测的更为短暂。BTN 在脂滴中的高流动性使其成为乳中潜在的可移动信号分子。

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