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Lipids activate SecA for high affinity binding to the SecYEG complex

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posted on 2024-11-15, 00:17 authored by Sabrina Koch, Janny De Wit, Iuliia Vos, Jan Birkner, Pavlo Gordiichuk, Andreas Herrmann, Antonius van OijenAntonius van Oijen, Arnold J Driessen
Protein translocation across the bacterial cytoplasmic membraneis an essential process catalyzed predominantly bythe Sec translocase. This system consists of the membrane-embedded protein-conducting channel SecYEG, the motor ATPase SecA, and the heterotrimeric SecDFyajC membrane protein complex. Previous studies suggest that anionic lipids are essential for SecA activity and that the N terminus of SecA is capable of penetrating the lipid bilayer. The role of lipid binding, however, has remained elusive. By employing differently sized nanodiscs reconstituted with single SecYEG complexes and comprising varying amounts of lipids, we establish that SecA gains access to the SecYEG complex via a lipid-bound intermediate state, whereas acidic phospholipids allosterically activate SecA for ATP-dependent protein translocation.

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Citation

Koch, S., De Wit, J., Vos, I., Birkner, J., Gordiichuk, P., Herrmann, A., van Oijen, A. M. & Driessen, A. J. (2016). Lipids activate SecA for high affinity binding to the SecYEG complex. Journal of Biological Chemistry, 291 (43), 22534-22543.

Journal title

Journal of Biological Chemistry

Volume

291

Issue

43

Pagination

22534-22543

Language

English

RIS ID

110320

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