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Identification of seipin-linked factors that act as determinants of a lipid droplet subpopulation

机译:鉴定脂质液滴亚贫化的决定因素的Seipin联系因子

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Functional heterogeneity within the lipid droplet (LD) pool of a single cell has been observed, yet the underlying mechanisms remain enigmatic. Here, we report on identification of a specialized LD subpopulation characterized by a unique proteome and a defined geographical location at the nucleus–vacuole junction contact site. In search for factors determining identity of these LDs, we screened ~6,000 yeast mutants for loss of targeting of the subpopulation marker Pdr16 and identified Ldo45 (LD organization protein of 45 kD) as a crucial targeting determinant. Ldo45 is the product of a splicing event connecting two adjacent genes ( YMR147W and YMR148W/OSW5/LDO16 ). We show that Ldo proteins cooperate with the LD biogenesis component seipin and establish LD identity by defining positioning and surface-protein composition. Our studies suggest a mechanism to establish functional differentiation of organelles, opening the door to better understanding of metabolic decisions in cells.
机译:已经观察到脂质液滴(LD)池内的功能异质性,但是底层机构保持神秘。在这里,我们报告了特征在于由核 - 漂浮结接触部位的独特蛋白质组和定义地理位置的专用LD亚群的鉴定。在寻找确定这些LDS的标识的因素中,我们筛选〜6,000酵母突变体,用于丢失亚潜疱疹标记PDR16的靶向,并确定LDO45(LD组织蛋白为45 kd)作为至关重要的靶向决定簇。 LDO45是连接两个相邻基因(YMR147W和YMR148W / OSW5 / LDO16)的拼接事件的乘积。我们表明LDO蛋白与LD生物发生成分Seipin合作,并通过定位定位和表面蛋白质组合物来建立LD同一性。我们的研究表明,建立有机细胞功能的功能分化,打开门,以更好地了解细胞中的代谢决策。

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