首页> 外文OA文献 >Autophagy-related Protein 8 (Atg8) Family Interacting Motif in Atg3 Mediates the Atg3-Atg8 Interaction and Is Crucial for the Cytoplasm-to-Vacuole Targeting Pathway*
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Autophagy-related Protein 8 (Atg8) Family Interacting Motif in Atg3 Mediates the Atg3-Atg8 Interaction and Is Crucial for the Cytoplasm-to-Vacuole Targeting Pathway*

机译:Atg3中的自噬相关蛋白8(Atg8)家族相互作用基序介导了Atg3-Atg8相互作用,对于细胞质至液泡的靶向通路至关重要*

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摘要

The autophagy-related protein 8 (Atg8) conjugation system is essential for the formation of double-membrane vesicles called autophagosomes during autophagy, a bulk degradation process conserved among most eukaryotes. It is also important in yeast for recognizing target vacuolar enzymes through the receptor protein Atg19 during the cytoplasm-to-vacuole targeting (Cvt) pathway, a selective type of autophagy. Atg3 is an E2-like enzyme that conjugates Atg8 with phosphatidylethanolamine. Here, we show that Atg3 directly interacts with Atg8 through the WEDL sequence, which is distinct from canonical interaction between E2 and ubiquitin-like modifiers. Moreover, NMR experiments suggest that the mode of interaction between Atg8 and Atg3 is quite similar to that between Atg8/LC3 and the Atg8 family interacting motif (AIM) conserved in autophagic receptors, such as Atg19 and p62. Thus, the WEDL sequence in Atg3 is a canonical AIM. In vitro analyses showed that Atg3 AIM is crucial for the transfer of Atg8 from the Atg8∼Atg3 thioester intermediate to phosphatidylethanolamine but not for the formation of the intermediate. Intriguingly, in vivo experiments showed that it is necessary for the Cvt pathway but not for starvation-induced autophagy. Atg3 AIM attenuated the inhibitory effect of Atg19 on Atg8 lipidation in vitro, suggesting that Atg3 AIM may be important for the lipidation of Atg19-bound Atg8 during the Cvt pathway.
机译:自噬相关蛋白8(Atg8)的缀合系统对于自噬过程中双膜囊泡(称为自噬体)的形成至关重要,这是大多数真核生物中所保留的整体降解过程。在酵母中,对于在细胞质至真空靶向(Cvt)途径(一种自噬的选择性途径)中通过受体蛋白Atg19识别靶液泡酶也很重要。 Atg3是一种类似E2的酶,可将Atg8与磷脂酰乙醇胺偶联。在这里,我们显示Atg3通过WEDL序列直接与Atg8相互作用,这与E2和泛素样修饰剂之间的规范相互作用不同。此外,NMR实验表明,Atg8和Atg3之间的相互作用模式与Atg8 / LC3和自噬受体(如Atg19和p62)中保守的Atg8家族相互作用基序(AIM)之间的相互作用模式非常相似。因此,Atg3中的WEDL序列是规范的AIM。体外分析表明,Atg3 AIM对于Atg8从Atg8〜Atg3硫代酯中间体向磷脂酰乙醇胺的转移至关重要,但对于中间体的形成并不重要。有趣的是,体内实验表明Cvt途径是必需的,但饥饿诱导的自噬则不需要。 Atg3 AIM在体外减弱了Atg19对Atg8脂质化的抑制作用,表明Atg3 AIM在Cvt途径中可能对与Atg19结合的Atg8的脂质化具有重要作用。

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