Litcius/Paper detail

Architecture and conformational dynamics of the BAM-SurA holo insertase complex

Philippe A. Lehner, Morris Degen, Roman P. Jakob, Seyed Majed Modaresi, Morgane Callon, Björn M. Burmann, Timm Maier, Sebastian Hiller

2025Science Advances14 citationsDOIOpen Access PDF

Abstract

The proper folding of outer membrane proteins in Gram-negative bacteria relies on their delivery to the β-barrel assembly machinery (BAM) complex. The mechanism by which survival protein A (SurA), the major periplasmic chaperone, facilitates this process is not well understood. We determine the structure of the holo insertase complex, where SurA binds BAM for substrate delivery. High-resolution cryo-electron microscopy structures of four different states and a three-dimensional variability analysis show that the holo insertase complex has a large motional spectrum. SurA bound to BAM can undergo a large swinging motion between two states. This motion is uncoupled from the conformational flexibility of the BamA barrel, which can open and close without affecting SurA binding. Notably, we observed conformational coupling of the SurA swing state and the carboxyl-terminal helix grip domain of BamC. Substrate delivery by SurA to BAM appears to follow a concerted motion that encodes a gated delivery pathway through the BAM accessory proteins to the membrane entry site.

Topics & Concepts

Periplasmic spaceBamaBiophysicsProtein structureChaperone (clinical)Conformational changeChemistryMolecular dynamicsBacterial outer membraneCell biologyCrystallographyBiologyBiochemistryEscherichia coliComputational chemistryGeneMedicinePathologyBacterial Genetics and BiotechnologyProtein Structure and DynamicsEnzyme Structure and Function
Architecture and conformational dynamics of the BAM-SurA holo insertase complex | Litcius