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Dissecting the mechanism of atlastin-mediated homotypic membrane fusion at the single-molecule level

Author

Listed:
  • Lijun Shi

    (Nankai University)

  • Chenguang Yang

    (Chinese Academy of Sciences
    University of Chinese Academy of Sciences)

  • Mingyuan Zhang

    (Zhejiang University)

  • Kangning Li

    (Nankai University)

  • Keying Wang

    (Zhejiang University)

  • Li Jiao

    (Nankai University)

  • Ruming Liu

    (Nankai University)

  • Yunyun Wang

    (Nankai University)

  • Ming Li

    (Chinese Academy of Sciences)

  • Yong Wang

    (Zhejiang University
    International Campus of Zhejiang University)

  • Lu Ma

    (Chinese Academy of Sciences)

  • Shuxin Hu

    (Chinese Academy of Sciences)

  • Xin Bian

    (Nankai University)

Abstract

Homotypic membrane fusion of the endoplasmic reticulum (ER) is mediated by dynamin-like GTPase atlastin (ATL). This fundamental process relies on GTP-dependent domain rearrangements in the N-terminal region of ATL (ATLcyto), including the GTPase domain and three-helix bundle (3HB). However, its conformational dynamics during the GTPase cycle remain elusive. Here, we combine single-molecule FRET imaging and molecular dynamics simulations to address this conundrum. Different from the prevailing model, ATLcyto can form a loose crossover dimer upon GTP binding, which is tightened by GTP hydrolysis for membrane fusion. Furthermore, the α-helical motif between the 3HB and transmembrane domain, which is embedded in the surface of the lipid bilayer and self-associates in the crossover dimer, is required for ATL function. To recycle the proteins, Pi release, which disassembles the dimer, activates frequent relative movements between the GTPase domain and 3HB, and subsequent GDP dissociation alters the conformational preference of the ATLcyto monomer for entering the next reaction cycle. Finally, we found that two disease-causing mutations affect human ATL1 activity by destabilizing GTP binding-induced loose crossover dimer formation and the membrane-embedded helix, respectively. These results provide insights into ATL-mediated homotypic membrane fusion and the pathological mechanisms of related disease.

Suggested Citation

  • Lijun Shi & Chenguang Yang & Mingyuan Zhang & Kangning Li & Keying Wang & Li Jiao & Ruming Liu & Yunyun Wang & Ming Li & Yong Wang & Lu Ma & Shuxin Hu & Xin Bian, 2024. "Dissecting the mechanism of atlastin-mediated homotypic membrane fusion at the single-molecule level," Nature Communications, Nature, vol. 15(1), pages 1-14, December.
    • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-46919-z
    DOI: 10.1038/s41467-024-46919-z
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    References listed on IDEAS

    as
    1. Genny Orso & Diana Pendin & Song Liu & Jessica Tosetto & Tyler J. Moss & Joseph E. Faust & Massimo Micaroni & Anastasia Egorova & Andrea Martinuzzi & James A. McNew & Andrea Daga, 2009. "Homotypic fusion of ER membranes requires the dynamin-like GTPase Atlastin," Nature, Nature, vol. 460(7258), pages 978-983, August.
    2. Xianzhuang Liu & Xiangyang Guo & Liling Niu & Xixia Li & Fei Sun & Junjie Hu & Xiangming Wang & Kang Shen, 2019. "Atlastin-1 regulates morphology and function of endoplasmic reticulum in dendrites," Nature Communications, Nature, vol. 10(1), pages 1-15, December.
    3. Mu Gao & Davi Nakajima An & Jerry M. Parks & Jeffrey Skolnick, 2022. "AF2Complex predicts direct physical interactions in multimeric proteins with deep learning," Nature Communications, Nature, vol. 13(1), pages 1-13, December.
    4. Alexander Stein & Gert Weber & Markus C. Wahl & Reinhard Jahn, 2009. "Helical extension of the neuronal SNARE complex into the membrane," Nature, Nature, vol. 460(7254), pages 525-528, July.
    5. Yang Chen & Lei Zhang & Laura Graf & Bing Yu & Yue Liu & Georg Kochs & Yongfang Zhao & Song Gao, 2017. "Conformational dynamics of dynamin-like MxA revealed by single-molecule FRET," Nature Communications, Nature, vol. 8(1), pages 1-11, August.
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