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Structures of the atlastin GTPase provide insight into homotypic fusion of endoplasmic reticulum membranes

Proceedings of the National Academy of Sciences2011Vol. 108(10), pp. 3976–3981

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Xin Bian, Robin W. Klemm, Tina Y. Liu, Miao Zhang, Sha Sun, Xuewu Sui, Xinqi Liu, Tom A. Rapoport, Junjie Hu

Abstract

The generation of the tubular network of the endoplasmic reticulum (ER) requires homotypic membrane fusion that is mediated by the dynamin-like, membrane-bound GTPase atlastin (ATL). Here, we have determined crystal structures of the cytosolic segment of human ATL1, which give insight into the mechanism of membrane fusion. The structures reveal a GTPase domain and athree-helix bundle, connected by a linker region. One structure corresponds to a prefusion state, in which ATL molecules in apposing membranes interact through their GTPase domains to form a dimer with the nucleotides bound at the interface. The other structure corresponds to a postfusion state generated after GTP hydrolysis and phosphate release. Compared with the prefusion structure, the three-helix bundles of the two ATL molecules undergo a major conformational change relative to the GTPase domains, which could pull the membranes together. The proposed fusion mechanism is supported by biochemical experiments and fusion assays with wild-type and mutant full-length Drosophila ATL. These experiments also show that membrane fusion is facilitated by the C-terminal cytosolic tails following the two transmembrane segments. Finally, our results show that mutations in ATL1 causing hereditary spastic paraplegia compromise homotypic ER fusion.

Citations Over TimeTop 10% of 2011 papers

Abstract

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