2020
DOI: 10.1111/febs.15309
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Membrane translocation at the ER: with a little help from my friends

Abstract: The Sec61 complex is the proteinaceous pore through which one-third of mammalian polypeptides access the lumen of the endoplasmic reticulum (ER) during their translocation across, or insertion into, the ER membrane. N-terminal ER signal peptides mediate polypeptide targeting to, and opening of, the Sec61 channel in a substrate-specific manner. Here, we discuss the recently defined features of ER signal peptides which necessitate the use of the accessory components Sec62 and Sec63 during the Sec61-mediated cotr… Show more

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Cited by 13 publications
(19 citation statements)
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“…This could mean that the cleaved cargo is passed to one or more intermediate factors post plasmepsin V cleavage before being taken by HSP101, or alternatively, HSP101 competes with plasmepsin V for cargo binding. A alternative explanation could also be proposed, where HSP101 binds to cargo prior to plasmepsin V cleavage, perhaps through interaction with the ER import translocon [23, 56], and releases it momentarily for plasmepsin V to cleave the PEXEL motif before immediately resuming its interaction with the mature cargo.…”
Section: Discussionmentioning
confidence: 99%
“…This could mean that the cleaved cargo is passed to one or more intermediate factors post plasmepsin V cleavage before being taken by HSP101, or alternatively, HSP101 competes with plasmepsin V for cargo binding. A alternative explanation could also be proposed, where HSP101 binds to cargo prior to plasmepsin V cleavage, perhaps through interaction with the ER import translocon [23, 56], and releases it momentarily for plasmepsin V to cleave the PEXEL motif before immediately resuming its interaction with the mature cargo.…”
Section: Discussionmentioning
confidence: 99%
“…Once substrates with special requirements start the gating process, Sec61β allows rapid integration of Sec63 into the active translocon. If so, Sec61β and Sec63 eventually will show a partially overlapping substrate-spectrum, which remains to be seen [ 6 , 18 , 67 ]. This scenario is reminiscent of a previous report showing the recruitment of the signal peptidase complex to the active, ribosome-engaged translocon by Sec61β [ 68 ].…”
Section: Discussionmentioning
confidence: 99%
“…One of the organelles that supports both intracellular signaling, for example calcium (Ca 2+ ) signaling or the unfolded protein response, and secretion of proteohormones is the endoplasmic reticulum (ER) [ 1 , 2 , 3 , 4 ]. A major membrane protein at the crossroad of ER signaling and protein transport is the heterotrimeric Sec61 complex acting as the pore-forming component of the ER protein translocase [ 5 , 6 , 7 ].…”
Section: Introductionmentioning
confidence: 99%
“…However, there is now a growing body of evidence that signal sequences can provide an additional, as yet poorly defined, level of control during membrane translocation [62]. Highly diverse in terms of their hydrophobicity, length, charge and specific amino acid composition [8,13,63], ER targeting signals appear to regulate the opening, or 'gating' of the Sec61 translocon [62], particularly since SRP effectively caters for targeting signals seemingly irrespective of their intrinsic ability to gate the translocon which, in some cases, is 'inefficient' and 'slow' (Fig. 3C) [64,65].…”
Section: Gating Of the Sec61 Complexmentioning
confidence: 99%
“…Furthermore, given that different gating assistants can contribute to the efficient translocation of the same protein substrate, whether a secretory protein or TMP (Fig. 3Ei, Tables 1-4) [74], and cellular levels of TRAP-b are upregulated following depletion of Sec62 [74], it seems likely that the TRAP complex and Sec62/Sec63 perform overlapping, but nonidentical, functions during Sec61-mediated protein translocation [62].…”
Section: Gating Of the Sec61 Complexmentioning
confidence: 99%