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Literature DB >> 29247569

Penetration into membrane of amino-terminal region of SecA when associated with SecYEG in active complexes.

Bahar T Findik¹, Virginia F Smith², Linda L Randall¹.

Abstract

The general secretory (Sec) system of Escherichia coli translocates both periplasmic and outer membrane proteins through the cytoplasmic membrane. The pathway through the membrane is provided by a highly conserved translocon, which in E. coli comprises two heterotrimeric integral membrane complexes, SecY, SecE, and SecG (SecYEG), and SecD, SecF, and YajC (SecDF/YajC). SecA is an associated ATPase that is essential to the function of the Sec system. SecA plays two roles, it targets precursors to the translocon with the help of SecB and it provides energy via hydrolysis of ATP. SecA exists both free in the cytoplasm and integrally membrane associated. Here we describe details of association of the amino-terminal region of SecA with membrane. We use site-directed spin labelling and electron paramagnetic resonance spectroscopy to show that when SecA is co-assembled into lipids with SecYEG to yield highly active translocons, the N-terminal region of SecA penetrates the membrane and lies at the interface between the polar and the hydrophobic regions, parallel to the plane of the membrane at a depth of approximately 5 Å. When SecA is bound to SecYEG, preassembled into proteoliposomes, or nonspecifically bound to lipids in the absence of SecYEG, the N-terminal region penetrates more deeply (8 Å). Implications of partitioning of the SecA N-terminal region into lipids on the complex between SecB carrying a precursor and SecA are discussed.

Entities: Chemical Gene Species

Keywords: EPR; SecA; SecYEG proteoliposomes; depth in bilayer; power saturation; protein export; protein-lipid interactions

Mesh：

Substances：

Year: 2018 PMID： 29247569 PMCID： PMC5818754 DOI： 10.1002/pro.3362

Source DB: PubMed Journal: Protein Sci ISSN： 0961-8368 Impact factor: 6.725

56 in total

1. Projection structure and oligomeric properties of a bacterial core protein translocase.

Authors: I Collinson; C Breyton; F Duong; C Tziatzios; D Schubert; E Or; T Rapoport; W Kühlbrandt
Journal: EMBO J Date: 2001-05-15 Impact factor: 11.598

2. Structural determinants of SecB recognition by SecA in bacterial protein translocation.

Authors: Jiahai Zhou; Zhaohui Xu
Journal: Nat Struct Biol Date: 2003-09-28

3. Dimeric SecA is essential for protein translocation.

Authors: Lucia B Jilaveanu; Christopher R Zito; Donald Oliver
Journal: Proc Natl Acad Sci U S A Date: 2005-05-16 Impact factor: 11.205

4. Export chaperone SecB uses one surface of interaction for diverse unfolded polypeptide ligands.

Authors: Angela A Lilly; Jennine M Crane; Linda L Randall
Journal: Protein Sci Date: 2009-09 Impact factor: 6.725

5. A significant fraction of functional SecA is permanently embedded in the membrane. SecA cycling on and off the membrane is not essential during protein translocation.

Authors: X Chen; H Xu; P C Tai
Journal: J Biol Chem Date: 1996-11-22 Impact factor: 5.157

6. SecA alone can promote protein translocation and ion channel activity: SecYEG increases efficiency and signal peptide specificity.

Authors: Ying-hsin Hsieh; Hao Zhang; Bor-ruei Lin; Ningren Cui; Bing Na; Hsiuchin Yang; Chun Jiang; Sen-fang Sui; Phang C Tai
Journal: J Biol Chem Date: 2011-10-27 Impact factor: 5.157

7. SecA of Escherichia coli traverses lipid bilayer of phospholipid vesicles.

Authors: T Ahn; H Kim
Journal: Biochem Biophys Res Commun Date: 1994-08-30 Impact factor: 3.575

8. The basis of asymmetry in the SecA:SecB complex.

Authors: Yuying Suo; Simon J S Hardy; Linda L Randall
Journal: J Mol Biol Date: 2014-12-19 Impact factor: 5.469

9. Deep penetration of a portion of Escherichia coli SecA protein into model membranes is promoted by anionic phospholipids and by partial unfolding.

Authors: N D Ulbrandt; E London; D B Oliver
Journal: J Biol Chem Date: 1992-07-25 Impact factor: 5.157

Review 7. Towards a Quantitative Understanding of Protein-Lipid Bilayer Interactions at the Single Molecule Level: Opportunities and Challenges.

Authors: Gavin M King; Ioan Kosztin
Journal: J Membr Biol Date: 2020-11-16 Impact factor: 1.843

8. The SecA ATPase motor protein binds to Escherichia coli liposomes only as monomers.

Authors: Guillaume Roussel; Stephen H White
Journal: Biochim Biophys Acta Biomembr Date: 2020-05-19 Impact factor: 3.747

8 in total

Penetration into membrane of amino-terminal region of SecA when associated with SecYEG in active complexes.

1. Projection structure and oligomeric properties of a bacterial core protein translocase.

2. Structural determinants of SecB recognition by SecA in bacterial protein translocation.

3. Dimeric SecA is essential for protein translocation.

4. Export chaperone SecB uses one surface of interaction for diverse unfolded polypeptide ligands.

5. A significant fraction of functional SecA is permanently embedded in the membrane. SecA cycling on and off the membrane is not essential during protein translocation.

6. SecA alone can promote protein translocation and ion channel activity: SecYEG increases efficiency and signal peptide specificity.

7. SecA of Escherichia coli traverses lipid bilayer of phospholipid vesicles.

8. The basis of asymmetry in the SecA:SecB complex.

9. Deep penetration of a portion of Escherichia coli SecA protein into model membranes is promoted by anionic phospholipids and by partial unfolding.

10. Lipids Activate SecA for High Affinity Binding to the SecYEG Complex.

1. Substrate Proteins Take Shape at an Improved Bacterial Translocon.

2. Binding of SecA ATPase monomers and dimers to lipid vesicles.

3. Direct visualization of the E. coli Sec translocase engaging precursor proteins in lipid bilayers.

4. Structure of the substrate-engaged SecA-SecY protein translocation machine.

5. Molecular Mimicry of SecA and Signal Recognition Particle Binding to the Bacterial Ribosome.

6. Interaction of the motor protein SecA and the bacterial protein translocation channel SecYEG in the absence of ATP.

Review 7. Towards a Quantitative Understanding of Protein-Lipid Bilayer Interactions at the Single Molecule Level: Opportunities and Challenges.

8. The SecA ATPase motor protein binds to Escherichia coli liposomes only as monomers.