The receptor subunit Tom20 is dynamically associated with the TOM complex in mitochondria of human cells

The outer membrane translocase (TOM) is the import channel for nuclear-encoded mitochondrial proteins. The general import pore contains Tom40, Tom22, Tom5, Tom6, and Tom7. Precursor proteins are bound by the (peripheral) receptor proteins Tom20, Tom22, and Tom70 before being imported by the TOM comp...

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Published inMolecular biology of the cell Vol. 32; no. 20; p. br1
Main Authors Bhagawati, Maniraj, Arroum, Tasnim, Webeling, Niklas, Montoro, Ayelén González, Mootz, Henning D, Busch, Karin B
Format Journal Article
LanguageEnglish
Published United States The American Society for Cell Biology 01.10.2021
Subjects
Brief Reports
HeLa Cells
Humans
Membrane Proteins - metabolism
Membrane Transport Proteins - metabolism
Mitochondria - metabolism
Mitochondrial Membrane Transport Proteins - metabolism
Mitochondrial Membranes - metabolism
Mitochondrial Precursor Protein Import Complex Proteins - genetics
Mitochondrial Precursor Protein Import Complex Proteins - metabolism
Mitochondrial Proteins - metabolism
Protein Transport
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Summary:The outer membrane translocase (TOM) is the import channel for nuclear-encoded mitochondrial proteins. The general import pore contains Tom40, Tom22, Tom5, Tom6, and Tom7. Precursor proteins are bound by the (peripheral) receptor proteins Tom20, Tom22, and Tom70 before being imported by the TOM complex. Here we investigated the association of the receptor Tom20 with the TOM complex. Tom20 was found in the TOM complex, but not in a smaller subcomplex. In addition, a subcomplex was found without Tom40 and Tom7 but with Tom20. Using single particle tracking of labeled Tom20 in overexpressing human cells, we show that Tom20 has, on average, higher lateral mobility in the membrane than Tom7/TOM. After ligation of Tom20 with the TOM complex by post-tranlational protein trans-splicing using the traceless, ultrafast cleaved Gp41-1 integrin system, a significant decrease in the mean diffusion coefficient of Tom20 was observed in the resulting Tom20-Tom7 fusion protein. Exposure of Tom20 to high substrate loading also resulted in reduced mobility. Taken together, our data show that the receptor subunit Tom20 interacts dynamically with the TOM core complex. We suggest that the TOM complex containing Tom20 is the active import pore and that Tom20 is associated when substrate is available.
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Data availability statement: data are available on request.
These authors contributed equally.
Conflicts of interest: The authors declare no conflict of interest.
Author contributions: conceptualization: K.B.B, M.B., T.A., A.G.M., and H.M.; methodology: K.B.B., N.W., T.A., M.B., A.G.M., and H.M.; validation: K.B.B., M.B., T.A., and A.G.M.; formal analysis: K.B.B., M.B., T.A., N.W., and A.G.M.; investigation: K.B.B., M.B., T.A., and A.G.M.; resources: K.B.B. and A.G.M.; writing—original draft preparation: K.B.B.; writing—review and editing: K.B.B., M.B., and H.M; visualization: T.A., M.B., A.G.M., and K.B.B.; supervision: K.B.B.; project administration: K.B.B.; funding acquisition: K.B.B. and H.M. All authors have read and agreed to the published version of the manuscript.
ISSN:1059-1524
1939-4586
DOI:10.1091/mbc.E21-01-0042