Atg38 is required for autophagy-specific phosphatidylinositol 3-kinase complex integrity

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Abstract

Autophagy is a conserved eukaryotic process of protein and organelle self-degradation within the vacuole/lysosome. Autophagy is characterized by the formation of an autophagosome, for which Vps34-dervied phosphatidylinositol 3-phosphate (PI3P) is essential. In yeast, Vps34 forms two distinct protein complexes: complex I, which functions in autophagy, and complex II, which is involved in protein sorting to the vacuole. Here we identify and characterize Atg38 as a stably associated subunit of complex I. In atg38δ cells, autophagic activity was significantly reduced and PI3-kinase complex I dissociated into the Vps15-Vps34 and Atg14-Vps30 subcomplexes. We find that Atg38 physically interacted with Atg14 and Vps34 via its N terminus. Further biochemical analyses revealed that Atg38 homodimerizes through its C terminus and that this homodimer formation is indispensable for the integrity of complex I. These data suggest that the homodimer of Atg38 functions as a physical linkage between the Vps15-Vps34 and Atg14-Vps30 subcomplexes to facilitate complex I formation. © 2013 Araki et al.

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APA

Araki, Y., Ku, W. C., Akioka, M., May, A. I., Hayashi, Y., Arisaka, F., … Ohsumi, Y. (2013). Atg38 is required for autophagy-specific phosphatidylinositol 3-kinase complex integrity. Journal of Cell Biology, 203(2), 299–313. https://doi.org/10.1083/jcb.201304123

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