Gram-negative trimeric porins have specific LPS binding sites that are essential for porin biogenesis

Arunmanee, Wanatchaporn; Pathania, M.; Solovyova, Alexandra S.; Brun, Anton P. Le; Ridley, Helen; Baslé, Arnaud; Berg, Bert van den; Lakey, Jeremy H.

doi:10.1073/pnas.1602382113

Cited by 107 publications

(108 citation statements)

References 67 publications

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“…The obtained results will be most interesting for studies of other porins with similar positively charged arginine ladders. Among these porins are the OmpF homologous or semihomologous OM Gram-negative bacterial proteins OmpC (68), PhoE (26), Omp32 (69), OmpK35/36 (70), OmpE35/ 36 (71), OprD (72), OprP (73), and OprO (74). Similar mechanisms as extracted here will likely apply, but especially for the narrower pores like OprD and OprP, the permeation rates will be much smaller than those for OmpF.…”

Section: Discussionmentioning

confidence: 68%

Fosfomycin Permeation through the Outer Membrane Porin OmpF

Golla

Sans-Serramitjana

Pothula

et al. 2019

Biophysical Journal

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Fosfomycin is a frequently prescribed drug in the treatment of acute urinary tract infections. It enters the bacterial cytoplasm and inhibits the biosynthesis of peptidoglycans by targeting the MurA enzyme. Despite extensive pharmacological studies and clinical use, the permeability of fosfomycin across the bacterial outer membrane is largely unexplored. Here, we investigate the fosfomycin permeability across the outer membrane of Gram-negative bacteria by electrophysiology experiments as well as by all-atom molecular dynamics simulations including free-energy and applied-field techniques. Notably, in an electrophysiological zero-current assay as well as in the molecular simulations, we found that fosfomycin can rapidly permeate the abundant Escherichia coli porin OmpF. Furthermore, two triple mutants in the constriction region of the porin have been investigated. The permeation rates through these mutants are slightly lower than that of the wild type but fosfomycin can still permeate. Altogether, this work unravels molecular details of fosfomycin permeation through the outer membrane porin OmpF of E. coli and moreover provides hints for understanding the translocation of phosphonic acid antibiotics through other outer membrane pores.

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Section: Discussionmentioning

confidence: 68%

Fosfomycin Permeation through the Outer Membrane Porin OmpF

Golla

Sans-Serramitjana

Pothula

et al. 2019

Biophysical Journal

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“…coli (Rocque et al, 1987;Strittmatter & Galanos, 1987;Buehler et al, 1991;de Cock & Tommassen, 1996), Salmonella (Strittmatter & Galanos, 1987;Latsch et al, 1992;Hagge et al, 2002) or Yersinia (Strittmatter & Galanos, 1987;Vakorina et al, 2003). This is well described for OmpF, a major porin of E. coli (Bolla et al, 1988;Holzenburg et al, 1989;Diedrich et al, 1990;Buehler et al, 1991;Sen & Nikaido, 1991;Arunmanee et al, 2014Arunmanee et al, , 2016Patel et al, 2016) belonging to the same family as Omp2b. One selective advantage of clustering R-LPS and Omp2b could be to facilitate diffusion of compounds from the medium into the pores of the porin, as suggested by theoretical simulations using OmpF as a model (Patel et al, 2016).…”

Section: Discussionmentioning

confidence: 60%

Localized incorporation of outer membrane components in the pathogen Brucella abortus

et al. 2019

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The zoonotic pathogen Brucella abortus is part of the Rhizobiales, which are alpha‐proteobacteria displaying unipolar growth. Here, we show that this bacterium exhibits heterogeneity in its outer membrane composition, with clusters of rough lipopolysaccharide co‐localizing with the essential outer membrane porin Omp2b, which is proposed to allow facilitated diffusion of solutes through the porin. We also show that the major outer membrane protein Omp25 and peptidoglycan are incorporated at the new pole and the division site, the expected growth sites. Interestingly, lipopolysaccharide is also inserted at the same growth sites. The absence of long‐range diffusion of main components of the outer membrane could explain the apparent immobility of the Omp2b clusters, as well as unipolar and mid‐cell localizations of newly incorporated outer membrane proteins and lipopolysaccharide. Unipolar growth and limited mobility of surface structures also suggest that new surface variants could arise in a few generations without the need of diluting pre‐existing surface antigens.

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“…Critical packing parameters are known for most of the glycerophospholipids, but until recently, only the structures of the unmodified hexa-acylated lipid A and its precursor from enterobacteria, lipid IV A , had been cocrystallized in certain membrane protein structures. A recent porin structure from the group of Jeremy Lakey has now revealed a hepta-acylated lipid A partial structure with C 16 esterified to the proximal glucosamine unit (13). As expected, the hepta-acylated lipid A has a larger cross-sectional molecular shape than its hexa-acylated counterpart, and it takes on a perceptible increase in conical shape.…”

Section: Commentarymentioning

confidence: 99%

Polymorphic Regulation of Outer Membrane Lipid A Composition

Bishop

2016

mBio

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The importance of the polymorphic-phase behavior of lipid A structural variations in determining their endotoxic activities has been recognized previously, but any potential role for lipid A polymorphism in controlling outer membrane structure and function has been largely ignored until now. In a recent article in mBio [7(5):e01532-16, https://doi.org/10.1128/mBio.01532-16], Katherine E. Bonnington and Meta J. Kuehn of Duke University’s Department of Biochemistry make a compelling case for considering how the molecular shapes of the various lipid A structural subtypes found in the outer membrane contribute to the process of outer membrane vesicle (OMV) formation.

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Gram-negative trimeric porins have specific LPS binding sites that are essential for porin biogenesis

Cited by 107 publications

References 67 publications

Fosfomycin Permeation through the Outer Membrane Porin OmpF

Fosfomycin Permeation through the Outer Membrane Porin OmpF

Localized incorporation of outer membrane components in the pathogen Brucella abortus

Polymorphic Regulation of Outer Membrane Lipid A Composition

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