The role of membrane destabilisation and protein dynamics in BAM catalysed OMP folding

Author:

White Paul,Haysom Samuel F.ORCID,Iadanza Matthew G.,Higgins Anna J.,Machin Jonathan M.,Whitehouse James M.,Horne Jim E.ORCID,Schiffrin Bob,Carpenter-Platt Charlotte,Calabrese Antonio N.ORCID,Storek Kelly M.,Rutherford Steven T.ORCID,Brockwell David J.ORCID,Ranson Neil A.ORCID,Radford Sheena E.ORCID

Abstract

AbstractThe folding of β-barrel outer membrane proteins (OMPs) in Gram-negative bacteria is catalysed by the β-barrel assembly machinery (BAM). How lateral opening in the β-barrel of the major subunit BamA assists in OMP folding, and the contribution of membrane disruption to BAM catalysis remain unresolved. Here, we use an anti-BamA monoclonal antibody fragment (Fab1) and two disulphide-crosslinked BAM variants (lid-locked (LL), and POTRA-5-locked (P5L)) to dissect these roles. Despite being lethal in vivo, we show that all complexes catalyse folding in vitro, albeit less efficiently than wild-type BAM. CryoEM reveals that while Fab1 and BAM-P5L trap an open-barrel state, BAM-LL contains a mixture of closed and contorted, partially-open structures. Finally, all three complexes globally destabilise the lipid bilayer, while BamA does not, revealing that the BAM lipoproteins are required for this function. Together the results provide insights into the role of BAM structure and lipid dynamics in OMP folding.

Funder

Wellcome Trust

RCUK | Medical Research Council

RCUK | Biotechnology and Biological Sciences Research Council

Royal Society

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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