In Close Proximity: The Lipid Droplet Proteome and Crosstalk With the Endoplasmic Reticulum.

Kirill Bersuker, James A Olzmann
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引用次数: 8

Abstract

Lipid droplets (LDs) are conserved, endoplasmic reticulum (ER)-derived organelles that act as a dynamic cellular repository for neutral lipids. Numerous studies have examined the composition of LD proteomes by using mass spectrometry to identify proteins present in biochemically isolated buoyant fractions that are enriched in LDs. Although many bona fide LD proteins were identified, high levels of non-LD proteins that contaminate buoyant fractions complicate the detection of true LD proteins. To overcome this problem, we recently developed a proximity-labeling proteomic method to define high-confidence LD proteomes. Moreover, employing this approach, we discovered that ER-associated degradation impacts the composition of LD proteomes by targeting select LD proteins for clearance by the 26S proteasome as they transit between the ER and LDs. These findings implicate the ER as a site of LD protein degradation and underscore the high degree of crosstalk between ER and LDs.

Abstract Image

近距离观察:脂滴蛋白质组与内质网的串扰。
脂滴(ld)是一种保守的内质网(ER)衍生的细胞器,作为中性脂质的动态细胞储存库。许多研究通过使用质谱法检测LD蛋白质组的组成,以鉴定存在于富含LD的生化分离浮力组分中的蛋白质。虽然鉴定了许多真正的LD蛋白,但高水平的非LD蛋白污染了浮力部分,使真正LD蛋白的检测复杂化。为了克服这个问题,我们最近开发了一种接近标记蛋白质组学方法来定义高置信度的LD蛋白质组。此外,采用这种方法,我们发现内质网相关的降解影响了LD蛋白质组的组成,通过靶向选择LD蛋白质,当它们在内质网和LD之间转运时,26S蛋白酶体将其清除。这些发现暗示内质网是LD蛋白降解的一个位点,并强调内质网和LD之间的高度串扰。
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