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A defect of the vacuolar putative lipase Atg15 accelerates degradation of lipid droplets through lipolysis

机译:液泡假定脂肪酶Atg15的缺陷通过脂解促进脂质液滴的降解。

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摘要

Lipid droplets (LDs) are the conserved organelles for the deposit of neutral lipids, and function as reservoirs of membrane and energy sources. To date, functional links between autophagy and LD dynamics have not been fully elucidated. Here, we report that a vacuolar putative lipase, Atg15, required for degradation of autophagic bodies, is crucial for the maintenance of LD amount in the yeast Saccharomyces cerevisiae in the stationary phase. Mutant analyses revealed that the putative lipase motif and vacuolar localization of Atg15 are important for the maintenance of LD amount. Loss of autophagosome formation by simultaneous deletion of core ATG genes cancelled the reduction in the LD amount in ATG15-deleted cells, indicating that degradation of autophagic bodies accounts for the functional involvement of Atg15 in LD dynamics. The reduced level of LDs in the mutant strain was dependent on Tgl3 and Tgl4, major lipases for lipolysis in S. cerevisiae. An altered phosphorylation status of Tgl3, higher accumulation of Tgl4, and closer associations of Tgl3 and Tgl4 with LDs were detected in the ATG15-deleted cells. Furthermore, increased levels of downstream metabolites of lipolysis in the mutant strain strongly suggested enhanced lipolytic activity caused by loss of ATG15. Our data provide evidence for a novel link between autophagic flux and LD dynamics integrated with Atg15 activity.
机译:脂质滴(LDs)是中性脂质沉积的保守细胞器,并起着膜和能量源的作用。迄今为止,自噬和LD动力学之间的功能联系尚未完全阐明。在这里,我们报道自噬体降解所需的液泡推定脂肪酶Atg15,对于维持固定期酿酒酵母中的LD量至关重要。突变分析表明,假定的脂肪酶基序和Atg15的液泡定位对维持LD量很重要。通过同时缺失核心ATG基因而导致的自噬体形成的丧失抵消了ATG15缺失细胞中LD量的减少,这表明自噬体的降解解释了Atg15在LD动力学中的功能性参与。突变菌株中LD的降低水平取决于Tgl3和Tgl4,这是酿酒酵母中脂解的主要脂肪酶。在缺失ATG15的细胞中检测到Tgl3的磷酸化状态改变,Tgl4的较高积累以及Tgl3和Tgl4与LD的紧密结合。此外,突变菌株中脂解的下游代谢产物水平升高强烈提示由ATG15丧失引起的脂解活性增强。我们的数据为自噬通量和与Atg15活性整合的LD动力学之间的新型联系提供了证据。

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