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Cryo-EM structures of S-OPA1 reveal its interactions with membrane and changes upon nucleotide binding.


ABSTRACT: Mammalian mitochondrial inner membrane fusion is mediated by optic atrophy 1 (OPA1). Under physiological conditions, OPA1 undergoes proteolytic processing to form a membrane-anchored long isoform (L-OPA1) and a soluble short isoform (S-OPA1). A combination of L-OPA1 and S-OPA1 is essential for efficient membrane fusion; however, the relevant mechanism is not well understood. In this study, we investigate the cryo-electron microscopic structures of S-OPA1-coated liposomes in nucleotide-free and GTP?S-bound states. S-OPA1 exhibits a general dynamin-like structure and can assemble onto membranes in a helical array with a dimer building block. We reveal that hydrophobic residues in its extended membrane-binding domain are critical for its tubulation activity. The binding of GTP?S triggers a conformational change and results in a rearrangement of the helical lattice and tube expansion similar to that of S-Mgm1. These observations indicate that S-OPA1 adopts a dynamin-like power stroke membrane remodeling mechanism during mitochondrial inner membrane fusion.

SUBMITTER: Zhang D 

PROVIDER: S-EPMC7156267 | biostudies-literature | 2020 Mar

REPOSITORIES: biostudies-literature

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Cryo-EM structures of S-OPA1 reveal its interactions with membrane and changes upon nucleotide binding.

Zhang Danyang D   Zhang Yan Y   Ma Jun J   Zhu Chunmei C   Niu Tongxin T   Chen Wenbo W   Pang Xiaoyun X   Zhai Yujia Y   Sun Fei F  

eLife 20200331


Mammalian mitochondrial inner membrane fusion is mediated by optic atrophy 1 (OPA1). Under physiological conditions, OPA1 undergoes proteolytic processing to form a membrane-anchored long isoform (L-OPA1) and a soluble short isoform (S-OPA1). A combination of L-OPA1 and S-OPA1 is essential for efficient membrane fusion; however, the relevant mechanism is not well understood. In this study, we investigate the cryo-electron microscopic structures of S-OPA1-coated liposomes in nucleotide-free and G  ...[more]

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