J Biol Chem. 2005 Dec 2;280(48):40058-65. Epub 2005 Sep 23.

Structural basis for the specificity and catalysis of human Atg4B responsible for mammalian autophagy.

Sugawara K, Suzuki NN, Fujioka Y, Mizushima N, Ohsumi Y, Inagaki F.

Department of Structural Biology, Graduate School of Pharmaceutical Sciences, Hokkaido University, N-12, W-6, Kita-ku, Sapporo 060-0812, Japan.

Reversible modification of Atg8 with phosphatidylethanolamine is crucial for autophagy, the bulk degradation system conserved in eukaryotic cells. Atg4 is a novel cysteine protease that processes and deconjugates Atg8. Herein, we report the crystal structure of human Atg4B (HsAtg4B) at 1.9-A resolution. Despite no obvious sequence homology with known proteases, the structure of HsAtg4B shows a classical papain-like fold. In addition to the papain fold region, HsAtg4B has a small alpha/beta-fold domain. This domain is thought to be the binding site for Atg8 homologs. The active site cleft of HsAtg4B is masked by a loop (residues 259-262), implying a conformational change upon substrate binding. The structure and in vitro mutational analyses provide the basis for the specificity and catalysis of HsAtg4B. This will enable the design of Atg4-specific inhibitors that block autophagy.

PMID: 16183633 [PubMed - indexed for MEDLINE]

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Structures reported by this article

The Crystal Structure Of Human Atg4b

PDB: 2CY7

Source: Homo sapiens

Method: X-Ray Diffraction | Resolution: 1.9 Å

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Structural basis for the specificity and catalysis of human Atg4B responsible for mammalian autophagy.

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