Literature DB >> 14536073

Cotranslational protein integration into the ER membrane is mediated by the binding of nascent chains to translocon proteins.

Peter J McCormick1, Yiwei Miao, Yuanlong Shao, Jialing Lin, Arthur E Johnson.   

Abstract

During cotranslational protein integration into the ER membrane, each transmembrane (TM) segment moves laterally through the translocon to reach the lipid bilayer. Photocrosslinking studies reveal that a particular surface of each nascent chain TM alpha helix and signal-anchor sequence always faces Sec61alpha in the translocon. This nonrandom and TM sequence-dependent positioning reveals that each TM segment makes specific contacts with Sec61alpha and is retained at a fixed location within the translocon, observations that are best explained by the binding of each TM sequence to a translocon protein(s). Since TM sequence hydrophobicity does not correlate with its rate of release from the translocon, nascent chain movement through the translocon appears to be mediated primarily by protein-protein interactions rather than hydrophobic nascent chain-phospholipid interactions.

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Year:  2003        PMID: 14536073     DOI: 10.1016/s1097-2765(03)00304-6

Source DB:  PubMed          Journal:  Mol Cell        ISSN: 1097-2765            Impact factor:   17.970


  48 in total

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9.  Translocation of a long amino-terminal domain through ER membrane by following signal-anchor sequence.

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