Membrane protein insertion through a mitochondrial β-barrel gate

Höhr, Alexandra I. C.; Lindau, Caroline; Wirth, Christophe; Qiu, Jian; Stroud, David A.; Kutik, Stephan; Guiard, Bernard; Hunte, Carola; Becker, Thomas; Pfanner, Nikolaus; Wiedemann, Nils

doi:10.1126/science.aah6834

Cited by 119 publications

(150 citation statements)

References 82 publications

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“…The β‐signal of the incoming precursor binds to the first β‐strand of Sam50 and thereby replaces the endogenous β‐signal of Sam50. The precursor stays at the lateral gate until the β‐barrel is folded . Sam50 may also stimulate the release of the precursor by distortion of the lipid bilayer as it was reported for the bacterial BamA .…”

Section: Channel‐forming Proteins In Protein Transportmentioning

confidence: 81%

“…Strikingly, addition of a β‐signal almost doubled the channel conductance to about 640 pS, indicating that the Sam50 channel pore is highly flexible. A recent study shows that the Sam50 channel is directly involved in protein insertion . Like the bacterial homolog BamA the β‐barrel of Sam50 forms a lateral gate between the first and the last β‐strand .…”

Section: Channel‐forming Proteins In Protein Transportmentioning

confidence: 99%

“…A recent study shows that the Sam50 channel is directly involved in protein insertion . Like the bacterial homolog BamA the β‐barrel of Sam50 forms a lateral gate between the first and the last β‐strand . Disulfide bond scanning reveals that the β‐barrel precursors are transferred via the channel lumen into the lateral gate of Sam50.…”

Section: Channel‐forming Proteins In Protein Transportmentioning

confidence: 99%

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Mitochondrial Outer Membrane Channels: Emerging Diversity in Transport Processes

Becker

Wagner

2018

BioEssays

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Mitochondrial function and biogenesis depend on the transport of a large variety of proteins, ions, and metabolites across the two surrounding membranes. While several specific transporters are present in the inner membrane, transport processes across the outer membrane are less understood. Recent studies reveal that the number of outer membrane channels and their transport mechanisms are more diverse than originally thought. Four protein-conducting channels promote transport of distinct sets of precursor proteins across and into the outer membrane. The voltage-dependent anion channel (VDAC) forms the major channel for small hydrophilic molecules. In addition, three channels with yet unknown substrate specificity exist in the outer membrane. In this review, we outline the emerging functional diversity, selectivity, and regulation of mitochondrial outer membrane channels. The presence of several channel-forming proteins challenges the traditional view that the outer membrane forms an unspecific size-exclusion filter for the flux of small hydrophilic molecules.

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Section: Channel‐forming Proteins In Protein Transportmentioning

confidence: 81%

Section: Channel‐forming Proteins In Protein Transportmentioning

confidence: 99%

Section: Channel‐forming Proteins In Protein Transportmentioning

confidence: 99%

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Mitochondrial Outer Membrane Channels: Emerging Diversity in Transport Processes

Becker

Wagner

2018

BioEssays

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“…There is reason to believe this is possible since the terminal β‐strands of Toc75 are structurally similar to the BamA/Sam50 homologs, which have weakly interacting terminal β‐strands . Recently, the mechanism of β‐barrel insertion via Sam50 was described wherein the first and last β‐strands of Sam50 pair with incoming substrate β‐strands . Once the substrate β‐barrel protein is fully inserted in the membrane, its terminal β‐strands would be paired with the terminal β‐strands of Sam50.…”

Section: Structural Considerations Of a Large Toc Complex Porementioning

confidence: 99%

Structural considerations of folded protein import through the chloroplast TOC/TIC translocons

Ganesan

Theg

2019

FEBS Letters

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Protein import into chloroplasts is carried out by the protein translocons at the outer and inner envelope membranes (TOC and TIC). Detailed structures for these translocons are lacking, with only a low‐resolution TOC complex structure available. Recently, we showed that the TOC/TIC translocons can import folded proteins, a rather unique feat for a coupled double membrane system. We also determined the maximum functional TOC/TIC pore size to be 30–35 Å. Here, we discuss how such large pores could form and compare the structural dynamics of the pore‐forming Toc75 subunit to its bacterial/mitochondrial Omp85 family homologs. We put forward structural models that can be empirically tested and also briefly review the pore dynamics of other protein translocons with known structures.

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“…The other Tom 39 proteins are associated with Tom40 by their single α-helical transmembrane segments (TMs). Although 40 functions of the α-helical Tom subunits are relatively poorly defined, they have been suggested to act either 41 as receptors for precursor proteins [16][17][18][19][20] or as binding sites for other factors 20,21 , and/or as escorts that 42 promote assembly and stability of the TOM complex 6,10,22,23 . 43 Current evidence indicates that translocation is a sequential process in which a precursor protein is first 44 recruited by the cytosolic receptor domains of Tom70, Tom20, and Tom22, then threaded into the pore of 45 Tom40, and finally handed over to the translocase of the inner membrane (TIM) complex or IMS-resident 46 chaperones (for review, see ref.…”

Section: Introduction 22mentioning

confidence: 99%

Cryo-EM structure of the mitochondrial protein-import channel TOM complex from Saccharomyces cerevisiae

Tucker¹,

Park

2019

Preprint

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9Nearly all mitochondrial proteins are encoded by the nuclear genome and imported into mitochondria 10 following synthesis on cytosolic ribosomes. These precursor proteins are translocated into mitochondria 11 by the TOM complex, a protein-conducting channel in the mitochondrial outer membrane. Using cryo-EM, 12we have obtained high-resolution structures of both apo and presequence-bound core TOM complexes 13from Saccharomyces cerevisiae in dimeric and tetrameric forms. Dimeric TOM consists of two copies each of 14 five proteins arranged in two-fold symmetry-Tom40, a pore-forming β-barrel with an overall negatively-15 charged inner surface, and four auxiliary α-helical transmembrane proteins. The structure suggests that 16 presequences for mitochondrial targeting insert into the Tom40 channel mainly by electrostatic and polar 17interactions. The tetrameric complex is essentially a dimer of dimeric TOM, which may be capable of 18forming higher-order oligomers. Our study reveals the molecular organization of the TOM complex and 19provides new insights about the mechanism of protein translocation into mitochondria. 20 21

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Membrane protein insertion through a mitochondrial β-barrel gate

Cited by 119 publications

References 82 publications

Mitochondrial Outer Membrane Channels: Emerging Diversity in Transport Processes

Mitochondrial Outer Membrane Channels: Emerging Diversity in Transport Processes

Structural considerations of folded protein import through the chloroplast TOC/TIC translocons

Cryo-EM structure of the mitochondrial protein-import channel TOM complex from Saccharomyces cerevisiae

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