SlyB encapsulates outer membrane proteins in stress-induced lipid nanodomains

Arne Janssens; Van Son Nguyen; Adam J Cecil; Sander E Van der Verren; Evy Timmerman; Michaël Deghelt; Alexander J Pak; Jean-François Collet; Francis Impens; Han Remaut

doi:10.1038/s41586-023-06925-5

SlyB encapsulates outer membrane proteins in stress-induced lipid nanodomains

Arne Janssens, Van Son Nguyen, Adam J Cecil, Sander E Van der Verren, Evy Timmerman, Michaël Deghelt, Alexander J Pak, Jean-François Collet, Francis Impens, Han Remaut

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Abstract

The outer membrane in Gram-negative bacteria consists of an asymmetric phospholipid-lipopolysaccharide bilayer that is densely packed with outer-membrane β-barrel proteins (OMPs) and lipoproteins1. The architecture and composition of this bilayer is closely monitored and is essential to cell integrity and survival2-4. Here we find that SlyB, a lipoprotein in the PhoPQ stress regulon, forms stable stress-induced complexes with the outer-membrane proteome. SlyB comprises a 10 kDa periplasmic β-sandwich domain and a glycine zipper domain that forms a transmembrane α-helical hairpin with discrete phospholipid- and lipopolysaccharide-binding sites. After loss in lipid asymmetry, SlyB oligomerizes into ring-shaped transmembrane complexes that encapsulate β-barrel proteins into lipid nanodomains of variable size. We find that the formation of SlyB nanodomains is essential during lipopolysaccharide destabilization by antimicrobial peptides or acute cation shortage, conditions that result in a loss of OMPs and compromised outer-membrane barrier function in the absence of a functional SlyB. Our data reveal that SlyB is a compartmentalizing transmembrane guard protein that is involved in cell-envelope proteostasis and integrity, and suggest that SlyB represents a larger family of broadly conserved lipoproteins with 2TM glycine zipper domains with the ability to form lipid nanodomains.

Original language	English
Pages (from-to)	617-625
Number of pages	9
Journal	Nature
Volume	626
Issue number	7999
Early online date	11 Dec 2023
DOIs	https://doi.org/10.1038/s41586-023-06925-5
Publication status	Published - 15 Feb 2024

Bibliographical note

Funding Information:
We thank M. Fislage and A. Schröfel for assistance with data collection at the VIB-VUB facility for Bio Electron Cryogenic Microscopy (BECM); and E. Parthoens at VIB Ghent Imaging Core for assistance in confocal imaging. A.J. and V.S.N. are recipients of a PhD and senior post-doctoral fellowship of the Flanders Research Foundation (FWO; FWOTM903 and 12ZM421N, respectively). We acknowledge financial support from VIB, FWO EOS grant G0G0818N and FWO research infrastructure grant G0H5916N. A.J.C. and A.J.P. acknowledge support from the National Institute of Allergy and Infectious Diseases of the National Institutes of Health under grant R21AI168838.

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© 2023, The Author(s), under exclusive licence to Springer Nature Limited.

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title = "SlyB encapsulates outer membrane proteins in stress-induced lipid nanodomains",

abstract = "The outer membrane in Gram-negative bacteria consists of an asymmetric phospholipid-lipopolysaccharide bilayer that is densely packed with outer-membrane β-barrel proteins (OMPs) and lipoproteins1. The architecture and composition of this bilayer is closely monitored and is essential to cell integrity and survival2-4. Here we find that SlyB, a lipoprotein in the PhoPQ stress regulon, forms stable stress-induced complexes with the outer-membrane proteome. SlyB comprises a 10 kDa periplasmic β-sandwich domain and a glycine zipper domain that forms a transmembrane α-helical hairpin with discrete phospholipid- and lipopolysaccharide-binding sites. After loss in lipid asymmetry, SlyB oligomerizes into ring-shaped transmembrane complexes that encapsulate β-barrel proteins into lipid nanodomains of variable size. We find that the formation of SlyB nanodomains is essential during lipopolysaccharide destabilization by antimicrobial peptides or acute cation shortage, conditions that result in a loss of OMPs and compromised outer-membrane barrier function in the absence of a functional SlyB. Our data reveal that SlyB is a compartmentalizing transmembrane guard protein that is involved in cell-envelope proteostasis and integrity, and suggest that SlyB represents a larger family of broadly conserved lipoproteins with 2TM glycine zipper domains with the ability to form lipid nanodomains.",

author = "Arne Janssens and Nguyen, {Van Son} and Cecil, {Adam J} and {Van der Verren}, {Sander E} and Evy Timmerman and Micha{\"e}l Deghelt and Pak, {Alexander J} and Jean-Fran{\c c}ois Collet and Francis Impens and Han Remaut",

note = "Funding Information: We thank M. Fislage and A. Schr{\"o}fel for assistance with data collection at the VIB-VUB facility for Bio Electron Cryogenic Microscopy (BECM); and E. Parthoens at VIB Ghent Imaging Core for assistance in confocal imaging. A.J. and V.S.N. are recipients of a PhD and senior post-doctoral fellowship of the Flanders Research Foundation (FWO; FWOTM903 and 12ZM421N, respectively). We acknowledge financial support from VIB, FWO EOS grant G0G0818N and FWO research infrastructure grant G0H5916N. A.J.C. and A.J.P. acknowledge support from the National Institute of Allergy and Infectious Diseases of the National Institutes of Health under grant R21AI168838. Publisher Copyright: {\textcopyright} 2023, The Author(s), under exclusive licence to Springer Nature Limited.",

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AU - Janssens, Arne

AU - Nguyen, Van Son

AU - Cecil, Adam J

AU - Van der Verren, Sander E

AU - Timmerman, Evy

AU - Deghelt, Michaël

AU - Pak, Alexander J

AU - Collet, Jean-François

AU - Impens, Francis

AU - Remaut, Han

N1 - Funding Information: We thank M. Fislage and A. Schröfel for assistance with data collection at the VIB-VUB facility for Bio Electron Cryogenic Microscopy (BECM); and E. Parthoens at VIB Ghent Imaging Core for assistance in confocal imaging. A.J. and V.S.N. are recipients of a PhD and senior post-doctoral fellowship of the Flanders Research Foundation (FWO; FWOTM903 and 12ZM421N, respectively). We acknowledge financial support from VIB, FWO EOS grant G0G0818N and FWO research infrastructure grant G0H5916N. A.J.C. and A.J.P. acknowledge support from the National Institute of Allergy and Infectious Diseases of the National Institutes of Health under grant R21AI168838. Publisher Copyright: © 2023, The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2024/2/15

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N2 - The outer membrane in Gram-negative bacteria consists of an asymmetric phospholipid-lipopolysaccharide bilayer that is densely packed with outer-membrane β-barrel proteins (OMPs) and lipoproteins1. The architecture and composition of this bilayer is closely monitored and is essential to cell integrity and survival2-4. Here we find that SlyB, a lipoprotein in the PhoPQ stress regulon, forms stable stress-induced complexes with the outer-membrane proteome. SlyB comprises a 10 kDa periplasmic β-sandwich domain and a glycine zipper domain that forms a transmembrane α-helical hairpin with discrete phospholipid- and lipopolysaccharide-binding sites. After loss in lipid asymmetry, SlyB oligomerizes into ring-shaped transmembrane complexes that encapsulate β-barrel proteins into lipid nanodomains of variable size. We find that the formation of SlyB nanodomains is essential during lipopolysaccharide destabilization by antimicrobial peptides or acute cation shortage, conditions that result in a loss of OMPs and compromised outer-membrane barrier function in the absence of a functional SlyB. Our data reveal that SlyB is a compartmentalizing transmembrane guard protein that is involved in cell-envelope proteostasis and integrity, and suggest that SlyB represents a larger family of broadly conserved lipoproteins with 2TM glycine zipper domains with the ability to form lipid nanodomains.

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DO - 10.1038/s41586-023-06925-5

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JO - Nature

JF - Nature

IS - 7999

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SlyB encapsulates outer membrane proteins in stress-induced lipid nanodomains

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