| Literature DB >> 32348752 |
Kim Nguyen Doan1, Alexander Grevel1, Christoph U Mårtensson1, Lars Ellenrieder2, Nicolas Thornton2, Lena-Sophie Wenz2, Łukasz Opaliński2, Bernard Guiard3, Nikolaus Pfanner4, Thomas Becker5.
Abstract
The mitochondrial outer membrane contains integral proteins with α-helical membrane anchors or a transmembrane β-barrel. The translocase of the outer membrane (TOM) cooperates with the sorting and assembly machinery (SAM) in the import of β-barrel proteins, whereas the mitochondrial import (MIM) complex inserts precursors of multi-spanning α-helical proteins. Single-spanning proteins constitute more than half of the integral outer membrane proteins; however, their biogenesis is poorly understood. We report that the yeast MIM complex promotes the insertion of proteins with N-terminal (signal-anchored) or C-terminal (tail-anchored) membrane anchors. The MIM complex exists in three dynamic populations. MIM interacts with TOM to accept precursor proteins from the receptor Tom70. Free MIM complexes insert single-spanning proteins that are imported in a Tom70-independent manner. Finally, coupling of MIM and SAM promotes early assembly steps of TOM subunits. We conclude that the MIM complex is a major and versatile protein translocase of the mitochondrial outer membrane.Entities:
Keywords: MIM complex; SAM complex; TOM complex; mitochondria; outer membrane; protein assembly; protein sorting; protein translocase
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Year: 2020 PMID: 32348752 DOI: 10.1016/j.celrep.2020.107567
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423