Structures of Atg7-Atg3 and Atg7-Atg10 reveal noncanonical mechanisms of E2 recruitment by the autophagy E1 |
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| Authors: | Stephen E. Kaiser Yu Qiu Julie E. Coats Kai Mao Daniel J. Klionsky Brenda A. Schulman |
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| Affiliation: | 1.Department of Structural Biology; St. Jude Children’s Research Hospital; Memphis, TN, USA;2.Life Sciences Institute; University of Michigan; Ann Arbor, MI USA;3.Howard Hughes Medical Institute; St. Jude Children’s Research Hospital; Memphis, TN USA |
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| Abstract: | Central to most forms of autophagy are two ubiquitin-like proteins (UBLs), Atg8 and Atg12, which play important roles in autophagosome biogenesis, substrate recruitment to autophagosomes, and other aspects of autophagy. Typically, UBLs are activated by an E1 enzyme that (1) catalyzes adenylation of the UBL C terminus, (2) transiently covalently captures the UBL through a reactive thioester bond between the E1 active site cysteine and the UBL C terminus, and (3) promotes transfer of the UBL C terminus to the catalytic cysteine of an E2 conjugating enzyme. The E2, and often an E3 ligase enzyme, catalyzes attachment of the UBL C terminus to a primary amine group on a substrate. Here, we summarize our recent work reporting the structural and mechanistic basis for E1-E2 protein interactions in autophagy. |
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| Keywords: | Atg10 Atg12 Atg3 Atg7 Atg8 E1 enzyme E2 enzyme ubiquitin-like protein |
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