Department of Cell Biology, University Medical Center Utrecht, 3584 CX Utrecht, The Netherlands.
Curr Biol. 2012 Sep 11;22(17):1545-53. doi: 10.1016/j.cub.2012.06.029. Epub 2012 Jul 5.
The biogenesis of autophagosomes, the hallmark of autophagy, depends on the function of the autophagy-related (Atg) proteins and the generation of phosphatidylinositol-3-phosphate (PtdIns3P) at the phagophore assembly site (PAS), the location where autophagosomes arise. The current model is that PtdIns3P is involved primarily in the recruitment of Atg proteins to the PAS and that once an autophagosome is complete, the Atg machinery is released from its surface back into the cytoplasm and reused for the formation of new vesicles.
We have identified a PtdIns3P phosphatase, Ymr1, that is essential for the normal progression of both bulk and selective types of autophagy. This protein is recruited to the PAS at an early stage of formation of this structure through a process that requires both its GRAM domain and its catalytic activity. In the absence of Ymr1, Atg proteins fail to dissociate from the limiting membrane of autophagosomes, and these vesicles accumulate in the cytoplasm.
Our data thus reveal a key role for PtdIns3P turnover in the regulation of the late steps of autophagosome biogenesis and indicate that the disassembly of the Atg machinery from the surface of autophagosomes is a requisite for their fusion with the vacuole.
自噬体的生物发生是自噬的标志,依赖于自噬相关(Atg)蛋白的功能和在吞噬体组装位点(PAS)产生的磷脂酰肌醇-3-磷酸(PtdIns3P)。目前的模型是 PtdIns3P 主要参与 Atg 蛋白向 PAS 的募集,并且一旦自噬体完成,Atg 机制就会从其表面释放回细胞质中,并重新用于形成新的囊泡。
我们已经鉴定出一种 PtdIns3P 磷酸酶 Ymr1,它对批量和选择性自噬的正常进行都是必不可少的。该蛋白通过一种需要其 GRAM 结构域和催化活性的过程,在该结构形成的早期被招募到 PAS。在 Ymr1 缺失的情况下,Atg 蛋白无法从自噬体的限制膜上解离,这些囊泡在细胞质中积累。
因此,我们的数据揭示了 PtdIns3P 周转在调节自噬体生物发生的后期步骤中的关键作用,并表明 Atg 机制从自噬体表面的解组装是其与液泡融合的必要条件。
