Your search keyword '"Jason J. Paxman"' showing total 39 results

1. Unveiling the versatility of the thioredoxin framework: Insights from the structural examination of Francisella tularensis DsbA1

Author

Stephanie Penning, Yaoqin Hong, Taylor Cunliffe, Lilian Hor, Makrina Totsika, Jason J. Paxman, and Begoña Heras

Subjects

Thioredoxin protein, Disulphide bond: Oxidoreductase, Crystal structure, Redox biology, AlphaFold, Biotechnology, TP248.13-248.65

Abstract

In bacteria the formation of disulphide bonds is facilitated by a family of enzymes known as the disulphide bond forming (Dsb) proteins, which, despite low sequence homology, belong to the thioredoxin (TRX) superfamily. Among these enzymes is the disulphide bond-forming protein A (DsbA); a periplasmic thiol oxidase responsible for catalysing the oxidative folding of numerous cell envelope and secreted proteins. Pathogenic bacteria often contain diverse Dsb proteins with distinct functionalities commonly associated with pathogenesis. Here we investigate FtDsbA1, a DsbA homologue from the Gram-negative bacterium Francisella tularensis. Our study shows that FtDsbA1 shares a conserved TRX-like fold bridged by an alpha helical bundle showcased by all DsbA-like proteins. However, FtDsbA1 displays a highly unique variation on this structure, containing an extended and flexible N-terminus and secondary structural elements inserted within the core of the TRX fold itself, which together twist the overall DsbA-like architecture. Additionally, FtDsbA1 exhibits variations to the well conserved active site with an unusual dipeptide in the catalytic CXXC redox centre (CGKC), and a trans configuration for the conserved cis-proline loop, known for governing DsbA-substrate interactions. FtDsbA1’s redox properties are comparable to other DsbA enzymes, however, consistent with its atypical structure, functional analysis reveals FtDsbA1 has a high degree of substrate specificity suggesting a specialised role within F. tularensis’ oxidative folding pathway. Overall, this work underscores the remarkable malleability of the TRX catalytic core, a ubiquitous and ancestral protein fold. This not only contributes to broadening the structural and functional diversity seen within proteins utilising this core fold but will also enhance the accuracy of AI-driven protein structural prediction tools.

Published

2024

2. Bacterial suppressor-of-copper-sensitivity proteins exhibit diverse thiol-disulfide oxidoreductase cellular functions

Author

Yaoqin Hong, Jilong Qin, Lachlan Mitchell, Jason J. Paxman, Begoña Heras, and Makrina Totsika

Subjects

Biochemistry, Microbiology, Structural biology, Science

Abstract

Summary: Disulfide bond (Dsb) oxidoreductases involved in oxidative protein folding govern bacterial survival and virulence. Over the past decade, oligomerization has emerged as a potential factor that dictates oxidoreductase activities. To investigate the role of oligomerization, we studied three Dsb-like ScsC oxidoreductases involved in copper resistance: the monomeric Salmonella enterica StScsC, and the trimeric Proteus mirabilis PmScsC and Caulobacter crescentus CcScsC. For copper sequestration, ScsC proteins must remain in the reduced form. However, all three ScsC proteins exhibit both dithiol oxidation and disulfide reduction activity, despite structural differences and previously reported limited in vitro activity. Most ScsC reductase activity relies on interactions with E. coli DsbD reductase, while oxidase activity depends on environmental oxidation. Interestingly, engineered monomeric PmScsC interacts effectively with the E. coli DsbB oxidase, at the partial expense of its reductase activity. These findings highlight oligomerization of oxidoreductases as a steric hindrance strategy to block undesirable upstream oxidative interactions.

Published

2024

3. Crystal structure of a subtilisin-like autotransporter passenger domain reveals insights into its cytotoxic function

Author

Lilian Hor, Akila Pilapitiya, James A. McKenna, Santosh Panjikar, Marilyn A. Anderson, Mickaël Desvaux, Jason J. Paxman, and Begoña Heras

Subjects

Science

Abstract

Autotransporters are bacterial proteins that possess multiple activities associated with pathogenesis. Here the authors present the structure of the autotransporter subtilase Ssp from Serratia marcescens and show that its distinctive structural features are required for its cytotoxic function.

Published

2023

4. Variation of Antigen 43 self-association modulates bacterial compacting within aggregates and biofilms

Author

Julieanne L. Vo, Gabriela C. Martínez Ortiz, Makrina Totsika, Alvin W. Lo, Steven J. Hancock, Andrew E. Whitten, Lilian Hor, Kate M. Peters, Valentin Ageorges, Nelly Caccia, Mickaël Desvaux, Mark A. Schembri, Jason J. Paxman, and Begoña Heras

Subjects

Microbial ecology, QR100-130

Abstract

Abstract The formation of aggregates and biofilms enhances bacterial colonisation and infection progression by affording protection from antibiotics and host immune factors. Despite these advantages there is a trade-off, whereby bacterial dissemination is reduced. As such, biofilm development needs to be controlled to suit adaptation to different environments. Here we investigate members from one of largest groups of bacterial adhesins, the autotransporters, for their critical role in the assembly of bacterial aggregates and biofilms. We describe the structural and functional characterisation of autotransporter Ag43 variants from different Escherichia coli pathotypes. We show that specific interactions between amino acids on the contacting interfaces of adjacent Ag43 proteins drives a common mode of trans-association that leads to cell clumping. Furthermore, subtle variation of these interactions alters aggregation kinetics and the degree of compacting within cell clusters. Together, our structure–function investigation reveals an underlying molecular basis for variations in the density of bacterial communities.

Published

2022

5. Phylogenetic Classification and Functional Review of Autotransporters

Author

Kaitlin R. Clarke, Lilian Hor, Akila Pilapitiya, Joen Luirink, Jason J. Paxman, and Begoña Heras

Subjects

type V secretion system, virulence, bacterial pathogenesis, toxins, adhesins, secreted proteins, Immunologic diseases. Allergy, RC581-607

Abstract

Autotransporters are the core component of a molecular nano-machine that delivers cargo proteins across the outer membrane of Gram-negative bacteria. Part of the type V secretion system, this large family of proteins play a central role in controlling bacterial interactions with their environment by promoting adhesion to surfaces, biofilm formation, host colonization and invasion as well as cytotoxicity and immunomodulation. As such, autotransporters are key facilitators of fitness and pathogenesis and enable co-operation or competition with other bacteria. Recent years have witnessed a dramatic increase in the number of autotransporter sequences reported and a steady rise in functional studies, which further link these proteins to multiple virulence phenotypes. In this review we provide an overview of our current knowledge on classical autotransporter proteins, the archetype of this protein superfamily. We also carry out a phylogenetic analysis of their functional domains and present a new classification system for this exquisitely diverse group of bacterial proteins. The sixteen phylogenetic divisions identified establish sensible relationships between well characterized autotransporters and inform structural and functional predictions of uncharacterized proteins, which may guide future research aimed at addressing multiple unanswered aspects in this group of therapeutically important bacterial factors.

Published

2022

6. A Buried Water Network Modulates the Activity of the Escherichia coli Disulphide Catalyst DsbA

Author

Geqing Wang, Jilong Qin, Anthony D. Verderosa, Lilian Hor, Carlos Santos-Martin, Jason J. Paxman, Jennifer L. Martin, Makrina Totsika, and Begoña Heras

Subjects

thioredoxin, redox regulation, disulphide, protein folding, bacterial pathogenesis, Therapeutics. Pharmacology, RM1-950

Abstract

The formation of disulphide bonds is an essential step in the folding of many proteins that enter the secretory pathway; therefore, it is not surprising that eukaryotic and prokaryotic organisms have dedicated enzymatic systems to catalyse this process. In bacteria, one such enzyme is disulphide bond-forming protein A (DsbA), a thioredoxin-like thiol oxidase that catalyses the oxidative folding of proteins required for virulence and fitness. A large body of work on DsbA proteins, particularly Escherichia coli DsbA (EcDsbA), has demonstrated the key role that the Cys30-XX-Cys33 catalytic motif and its unique redox properties play in the thiol oxidase activity of this enzyme. Using mutational and functional analyses, here we identify that a set of charged residues, which form an acidic groove on the non-catalytic face of the enzyme, further modulate the activity of EcDsbA. Our high-resolution structures indicate that these residues form a water-mediated proton wire that can transfer protons from the bulk solvent to the active site. Our results support the view that proton shuffling may facilitate the stabilisation of the buried Cys33 thiolate formed during the redox reaction and promote the correct direction of the EcDsbA–substrate thiol–disulphide exchange. Comparison with other proteins of the same class and proteins of the thioredoxin-superfamily in general suggest that a proton relay system appears to be a conserved catalytic feature among this widespread superfamily of proteins. Furthermore, this study also indicates that the acidic groove of DsbA could be a promising allosteric site to develop novel DsbA inhibitors as antibacterial therapeutics.

Published

2023

7. Unique structural features of a bacterial autotransporter adhesin suggest mechanisms for interaction with host macromolecules

Author

Jason J. Paxman, Alvin W. Lo, Matthew J. Sullivan, Santosh Panjikar, Michael Kuiper, Andrew E. Whitten, Geqing Wang, Chi-Hao Luan, Danilo G. Moriel, Lendl Tan, Kate M. Peters, Minh-Duy Phan, Christine L. Gee, Glen C. Ulett, Mark A. Schembri, and Begoña Heras

Subjects

Science

Abstract

Autotransporter proteins are localised to the bacterial surface and promote colonisation of host epithelial surfaces. Here, the authors present the crystal structure of autotransporter UpaB and show evidence for distinct binding sites for glycosaminoglycans and host fibronectin.

Published

2019

8. Molecular and Structural Characterization of a Novel Escherichia coli Interleukin Receptor Mimic Protein

Author

Danilo G. Moriel, Begoña Heras, Jason J. Paxman, Alvin W. Lo, Lendl Tan, Matthew J. Sullivan, Samantha J. Dando, Scott A. Beatson, Glen C. Ulett, and Mark A. Schembri

Subjects

Microbiology, QR1-502

Abstract

ABSTRACT Urinary tract infection (UTI) is a disease of extremely high incidence in both community and nosocomial settings. UTIs cause significant morbidity and mortality, with approximately 150 million cases globally per year. Uropathogenic Escherichia coli (UPEC) is the primary cause of UTI and is generally treated empirically. However, the rapidly increasing incidence of UTIs caused by multidrug-resistant UPEC strains has led to limited available treatment options and highlights the urgent need to develop alternative treatment and prevention strategies. In this study, we performed a comprehensive analysis to define the regulation, structure, function, and immunogenicity of recently identified UPEC vaccine candidate C1275 (here referred to as IrmA). We showed that the irmA gene is highly prevalent in UPEC, is cotranscribed with the biofilm-associated antigen 43 gene, and is regulated by the global oxidative stress response OxyR protein. Localization studies identified IrmA in the UPEC culture supernatant. We determined the structure of IrmA and showed that it adopts a unique domain-swapped dimer architecture. The dimeric structure of IrmA displays similarity to those of human cytokine receptors, including the interleukin-2 receptor (IL-2R), interleukin-4 receptor (IL-4R), and interleukin-10 receptor (IL-10R) binding domains, and we showed that purified IrmA can bind to their cognate cytokines. Finally, we showed that plasma from convalescent urosepsis patients contains high IrmA antibody titers, demonstrating the strong immunogenicity of IrmA. Taken together, our results indicate that IrmA may play an important role during UPEC infection. IMPORTANCE Uropathogenic E. coli (UPEC) is the primary cause of urinary tract infection (UTI), a disease of major significance to human health. Globally, the incidence of UPEC-mediated UTI is strongly associated with increasing antibiotic resistance, making this extremely common infection a major public health concern. In this report, we describe the regulatory, structural, functional, and immunogenic properties of a candidate UPEC vaccine antigen, IrmA. We demonstrate that IrmA is a small UPEC protein that forms a unique domain-swapped dimer with structural mimicry to several human cytokine receptors. We also show that IrmA binds to IL-2, IL-4, and IL-10, is strongly immunogenic in urosepsis patients, and is coexpressed with factors associated with biofilm formation. Overall, this work suggests a potential novel contribution for IrmA in UPEC infection.

Published

2016

9. Targeting Bacterial Dsb Proteins for the Development of Anti-Virulence Agents

Author

Roxanne P. Smith, Jason J. Paxman, Martin J. Scanlon, and Begoña Heras

Subjects

disulfide catalysis, DsbA inhibitors, DsbB inhibitors, anti-virulence, fragment-based drug design, antimicrobial resistance, Organic chemistry, QD241-441

Abstract

Recent years have witnessed a dramatic increase in bacterial antimicrobial resistance and a decline in the development of novel antibiotics. New therapeutic strategies are urgently needed to combat the growing threat posed by multidrug resistant bacterial infections. The Dsb disulfide bond forming pathways are potential targets for the development of antimicrobial agents because they play a central role in bacterial pathogenesis. In particular, the DsbA/DsbB system catalyses disulfide bond formation in a wide array of virulence factors, which are essential for many pathogens to establish infections and cause disease. These redox enzymes are well placed as antimicrobial targets because they are taxonomically widespread, share low sequence identity with human proteins, and many years of basic research have provided a deep molecular understanding of these systems in bacteria. In this review, we discuss disulfide bond catalytic pathways in bacteria and their significance in pathogenesis. We also review the use of different approaches to develop inhibitors against Dsb proteins as potential anti-virulence agents, including fragment-based drug discovery, high-throughput screening and other structure-based drug discovery methods.

Published

2016

10. Bacterial suppressor-of-copper-sensitivity (Scs) proteins exhibit diverse thiol-disulfide oxidoreductase cellular functions

Author

Yaoqin Hong, Jilong Qin, Lachlan Mitchell, Jason J. Paxman, Begoña Heras, and Makrina Totsika

Abstract

Disulfide bond (Dsb) proteins catalyse oxidative protein folding governing bacterial survival and virulence. Dsb systems inEscherichia coliK-12 are well-studied, yet what determines dithiol oxidase or disulfide reductase activity remains unknown. Past studies suggest oligomerisation of periplasmic thiol oxidoreductases dictates the direction of thiol catalytic activity. Here, we studied three suppressor-of-copper-sensitivity C (ScsC) Dsb-like proteins known to exist in the reduced state and bind to copper. These proteins adopt different quaternary structures:Salmonella entericaScsC (StScsC) is monomeric, while ScsC fromProteus mirabilis(PmScsC) andCaulobacter crescentus(CcScsC) are trimeric. When expressed in the model organismE. coliK-12, we showed that all three ScsC proteins exhibit both dithiol oxidation and disulfide reduction activity, despite structural differences. Interestingly, while ScsC reductase function was supported by the canonicalE. coliDsbD reductase, oxidase activity depended on environmental oxidation. However, an engineered monomeric PmScsC synergises withE. coliDsbB to gain dithiol oxidase activity at the expense of reductase function. Thus, oligomerisation could be one mechanism by which ScsC proteins avoid interactions with the periplasmic thiol oxidase pathway. This tightly controls their re-oxidation and maintains ScsC proteins in the reduced state required for binding and sequestering toxic levels of cellular copper.

Published

2023

11. Inhibition of Diverse DsbA Enzymes in Multi-DsbA Encoding Pathogens

Author

Jason J. Paxman, Dimitrios Vagenas, Makrina Totsika, Jennifer L. Martin, Pooja Sharma, Geqing Wang, Martin J. Scanlon, Rabeb Dhouib, and Begoña Heras

Subjects

0301 basic medicine, Physiology, Clinical Biochemistry, Protein Disulfide-Isomerases, Virulence, Microbial Sensitivity Tests, Thiophenes, medicine.disease_cause, Biochemistry, Virulence factor, 03 medical and health sciences, protein folding, therapeutics, medicine, Enzyme Inhibitors, Molecular Biology, Escherichia coli, General Environmental Science, Uncategorized, chemistry.chemical_classification, Escherichia coli K12, biology, Chemistry, Escherichia coli Proteins, thiol, Active site, Cell Biology, biology.organism_classification, infection, Anti-Bacterial Agents, Original Research Communications, 030104 developmental biology, Enzyme, DsbA, Salmonella enterica, biology.protein, General Earth and Planetary Sciences, Bacterial outer membrane

Abstract

Aims: DsbA catalyzes disulfide bond formation in secreted and outer membrane proteins in bacteria. In pathogens, DsbA is a major facilitator of virulence constituting a target for antivirulence antimicrobial development. However, many pathogens encode multiple and diverse DsbA enzymes for virulence factor folding during infection. The aim of this study was to determine whether our recently identified inhibitors of Escherichia coli K-12 DsbA can inhibit the diverse DsbA enzymes found in two important human pathogens and attenuate their virulence. Results: DsbA inhibitors from two chemical classes (phenylthiophene and phenoxyphenyl derivatives) inhibited the virulence of uropathogenic E. coli and Salmonella enterica serovar Typhimurium, encoding two and three diverse DsbA homologues, respectively. Inhibitors blocked the virulence of dsbA null mutants complemented with structurally diverse DsbL and SrgA, suggesting that they were not selective for prototypical DsbA. Structural characterization of DsbA-inhibitor complexes showed that compounds from each class bind in a similar region of the hydrophobic groove adjacent to the Cys30-Pro31-His32-Cys33 (CPHC) active site. Modeling of DsbL- and SrgA-inhibitor interactions showed that these accessory enzymes could accommodate the inhibitors in their different hydrophobic grooves, supporting our in vivo findings. Further, we identified highly conserved residues surrounding the active site for 20 diverse bacterial DsbA enzymes, which could be exploited in developing inhibitors with a broad spectrum of activity. Innovation and Conclusion: We have developed tools to analyze the specificity of DsbA inhibitors in bacterial pathogens encoding multiple DsbA enzymes. This work demonstrates that DsbA inhibitors can be developed to target diverse homologues found in bacteria. Antioxid. Redox Signal. 29, 653–666.

Published

2023

12. Molecular and structural characterization of a novel Escherichia coli interleukin receptor mimic protein

Author

Begoña Heras, Samantha J. Dando, Mark A. Schembri, Jason J. Paxman, Glen C. Ulett, Matthew J. Sullivan, Scott A. Beatson, Lendl Tan, Danilo Gomes Moriel, and Alvin W. Lo

Subjects

0301 basic medicine, 030106 microbiology, Biology, urologic and male genital diseases, medicine.disease_cause, Microbiology, 03 medical and health sciences, Antigen, Virology, medicine, Humans, Uropathogenic Escherichia coli, Receptor, Escherichia coli, Uncategorized, Escherichia coli Proteins, Immunogenicity, Molecular Mimicry, Antibody titer, Receptors, Interleukin, 060500 MICROBIOLOGY, bacterial infections and mycoses, Antibodies, Bacterial, QR1-502, female genital diseases and pregnancy complications, 3. Good health, Molecular mimicry, 030104 developmental biology, biology.protein, Cytokines, Interleukin receptor, Antibody, Research Article

Abstract

Urinary tract infection (UTI) is a disease of extremely high incidence in both community and nosocomial settings. UTIs cause significant morbidity and mortality, with approximately 150 million cases globally per year. Uropathogenic Escherichia coli (UPEC) is the primary cause of UTI and is generally treated empirically. However, the rapidly increasing incidence of UTIs caused by multidrug-resistant UPEC strains has led to limited available treatment options and highlights the urgent need to develop alternative treatment and prevention strategies. In this study, we performed a comprehensive analysis to define the regulation, structure, function, and immunogenicity of recently identified UPEC vaccine candidate C1275 (here referred to as IrmA). We showed that the irmA gene is highly prevalent in UPEC, is cotranscribed with the biofilm-associated antigen 43 gene, and is regulated by the global oxidative stress response OxyR protein. Localization studies identified IrmA in the UPEC culture supernatant. We determined the structure of IrmA and showed that it adopts a unique domain-swapped dimer architecture. The dimeric structure of IrmA displays similarity to those of human cytokine receptors, including the interleukin-2 receptor (IL-2R), interleukin-4 receptor (IL-4R), and interleukin-10 receptor (IL-10R) binding domains, and we showed that purified IrmA can bind to their cognate cytokines. Finally, we showed that plasma from convalescent urosepsis patients contains high IrmA antibody titers, demonstrating the strong immunogenicity of IrmA. Taken together, our results indicate that IrmA may play an important role during UPEC infection., IMPORTANCE Uropathogenic E. coli (UPEC) is the primary cause of urinary tract infection (UTI), a disease of major significance to human health. Globally, the incidence of UPEC-mediated UTI is strongly associated with increasing antibiotic resistance, making this extremely common infection a major public health concern. In this report, we describe the regulatory, structural, functional, and immunogenic properties of a candidate UPEC vaccine antigen, IrmA. We demonstrate that IrmA is a small UPEC protein that forms a unique domain-swapped dimer with structural mimicry to several human cytokine receptors. We also show that IrmA binds to IL-2, IL-4, and IL-10, is strongly immunogenic in urosepsis patients, and is coexpressed with factors associated with biofilm formation. Overall, this work suggests a potential novel contribution for IrmA in UPEC infection.

Published

2023

13. Salmonella enterica BcfH Is a Trimeric Thioredoxin-Like Bifunctional Enzyme with Both Thiol Oxidase and Disulfide Isomerase Activities

Author

Yaoqin Hong, Jennifer L. Martin, Begoña Heras, Jason J. Paxman, Carlos F. Santos-Martin, Pramod Subedi, Santosh Panjikar, Anthony D. Verderosa, Geqing Wang, Lilian Hor, Makrina Totsika, and Andrew E. Whitten

Subjects

0301 basic medicine, chemistry.chemical_classification, 030102 biochemistry & molecular biology, Protein family, biology, Physiology, Oxidative folding, Clinical Biochemistry, Cell Biology, Biochemistry, 03 medical and health sciences, 030104 developmental biology, chemistry, Oxidoreductase, Thiol oxidase, biology.protein, General Earth and Planetary Sciences, Phosphofructokinase 2, Protein folding, Thioredoxin, Protein disulfide-isomerase, Molecular Biology, General Environmental Science

Abstract

Aims: Thioredoxin (TRX)-fold proteins are ubiquitous in nature. This redox scaffold has evolved to enable a variety of functions, including redox regulation, protein folding, and oxidative stress defense. In bacteria, the TRX-like disulfide bond (Dsb) family mediates the oxidative folding of multiple proteins required for fitness and pathogenic potential. Conventionally, Dsb proteins have specific redox functions with monomeric and dimeric Dsbs exclusively catalyzing thiol oxidation and disulfide isomerization, respectively. This contrasts with the eukaryotic disulfide forming machinery where the modular TRX protein disulfide isomerase (PDI) mediates thiol oxidation and disulfide reshuffling. In this study, we identified and structurally and biochemically characterized a novel Dsb-like protein from Salmonella enterica termed bovine colonization factor protein H (BcfH) and defined its role in virulence. Results: In the conserved bovine colonization factor (bcf) fimbrial operon, the Dsb-like enzyme BcfH forms a trimeric structure, exceptionally uncommon among the large and evolutionary conserved TRX superfamily. This protein also displays very unusual catalytic redox centers, including an unwound α-helix holding the redox active site and a trans-proline instead of the conserved cis-proline active site loop. Remarkably, BcfH displays both thiol oxidase and disulfide isomerase activities contributing to Salmonella fimbrial biogenesis. Innovation and Conclusion: Typically, oligomerization of bacterial Dsb proteins modulates their redox function, with monomeric and dimeric Dsbs mediating thiol oxidation and disulfide isomerization, respectively. This study demonstrates a further structural and functional malleability in the TRX-fold protein family. BcfH trimeric architecture and unconventional catalytic sites permit multiple redox functions emulating in bacteria the eukaryotic PDI dual oxidoreductase activity. Antioxid. Redox Signal. 35, 21-39.

Published

2021

14. Genome-Wide Analysis of Antigen 43 (Ag43) Variants: New Insights in Their Diversity, Distribution and Prevalence in Bacteria

Author

Valentin Ageorges, Ivan Wawrzyniak, Philippe Ruiz, Cédric Bicep, Mohamed A. Zorgani, Jason J. Paxman, Begoña Heras, Ian R. Henderson, Sabine Leroy, Xavier Bailly, Panagiotis Sapountzis, Eric Peyretaillade, Mickaël Desvaux, Microbiologie Environnement Digestif Santé (MEDIS), Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)-Université Clermont Auvergne (UCA), Laboratoire Microorganismes : Génome et Environnement (LMGE), Centre National de la Recherche Scientifique (CNRS)-Université Clermont Auvergne (UCA), La Trobe University, The University of Queensland, FIM2Lab – Functional Interfacial Materials and Membrane Laboratory, School of Chemical Engineering, Brisbane, QLD 4067, Australia (FIM2Lab), University of Queensland [Brisbane], Unité Mixte de Recherche d'Épidémiologie des maladies Animales et zoonotiques (UMR EPIA), and VetAgro Sup - Institut national d'enseignement supérieur et de recherche en alimentation, santé animale, sciences agronomiques et de l'environnement (VAS)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)

Subjects

Inorganic Chemistry, [SDV]Life Sciences [q-bio], Organic Chemistry, Escherichia coli, protein secretion, autotransporter, Type V protein secretion system (T5SS), phylogeny, gene diversity, bacterial pathogens, cell surface protein, aggregation, bacterial colonisation and infection and infection, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Uncategorized, Computer Science Applications

Abstract

Antigen 43 (Ag43) expression induces aggregation and biofilm formation that has consequences for bacterial colonisation and infection. Ag43 is secreted through the Type 5 subtype “a” secretion system (T5aSS) and is a prototypical member of the family of self-associating autotransporters (SAATs). As a T5aSS protein, Ag43 has a modular architecture comprised of (i) a signal peptide, (ii) a passenger domain that can be subdivided into three subdomains (SL, EJ, and BL), (iii) an autochaperone (AC) domain, and (iv) an outer membrane translocator. The cell-surface SL subdomain is directly involved in the “Velcro-handshake” mechanism resulting in bacterial autoaggregation. Ag43 is considered to have a ubiquitous distribution in E. coli genomes and many strains harbour multiple agn43 genes. However, recent phylogenetic analyses indicated the existence of four distinct Ag43 classes exhibiting different propensities for autoaggregation and interactions. Given the knowledge of the diversity and distribution of Ag43 in E. coli genomes is incomplete, we have performed a thorough in silico investigation across bacterial genomes. Our comprehensive analyses indicate that Ag43 passenger domains cluster in six phylogenetic classes associated with different SL subdomains. The diversity of Ag43 passenger domains is a result of the association of the SL subtypes with two different EJ-BL-AC modules. We reveal that agn43 is almost exclusively present among bacterial species of the Enterobacteriaceae family and essentially in the Escherichia genus (99.6%) but that it is not ubiquitous in E. coli. The gene is typically present as a single copy but up to five copies of agn43 with different combinations of classes can be observed. The presence of agn43 as well as its different classes appeared to differ between Escherichia phylogroups. Strikingly, agn43 is present in 90% of E. coli from E phylogroup. Our results shed light on Ag43 diversity and provide a rational framework for investigating its role in E. coli ecophysiology and physiopathology.

Published

2023

15. A Molecular Chameleon for Mapping Subcellular Polarity in an Unfolded Proteome Environment

Author

Yuning Hong, Elizabeth Hinde, Jason J. Paxman, Begoña Heras, Jonathan M. White, Weisan Chen, Wallace W. H. Wong, Pramod Subedi, Deng Jieru, and Tze Cin Owyong

Subjects

Cytoplasm, Proteome, Polarity (physics), 010402 general chemistry, 01 natural sciences, Catalysis, 03 medical and health sciences, medicine, Humans, Fluorescent Dyes, 030304 developmental biology, Cell Nucleus, 0303 health sciences, Chemistry, 010405 organic chemistry, HEK 293 cells, General Chemistry, General Medicine, 0104 chemical sciences, Cell nucleus, HEK293 Cells, medicine.anatomical_structure, Proteostasis, Drug Design, Unfolded Protein Response, Unfolded protein response, Biophysics, Nucleus

Abstract

Environmental polarity is an important factor that drives biomolecular interactions to regulate cell function. Herein, a general method of using the fluorogenic probe NTPAN-MI is reported to quantify the subcellular polarity change in response to protein unfolding. NTPAN-MI fluorescence is selectively activated upon labeling unfolded proteins with exposed thiols, thereby reporting on the extent of proteostasis. NTPAN-MI also reveals the collapse of the host proteome caused by influenza A virus infection. The emission profile of NTPAN-MI contains information of the local polarity of the unfolded proteome, which can be resolved through spectral phasor analysis. Under stress conditions that disrupt different checkpoints of protein quality control, distinct patterns of dielectric constant distribution in the cytoplasm can be observed. However, in the nucleus, the unfolded proteome was found to experience a more hydrophilic environment across all the stress conditions, indicating the central role of nucleus in the stress response process.

Published

2020

16. The Scs disulfide reductase system cooperates with the metallochaperone CueP in Salmonella copper resistance

Author

Geqing Wang, Pramod Subedi, Ashwinie A. Ukuwela, Jason J. Paxman, Begoña Heras, and Zhiguang Xiao

Subjects

0301 basic medicine, integumentary system, 030102 biochemistry & molecular biology, biology, Chemistry, Oxidative folding, Copper toxicity, Cell Biology, Periplasmic space, Oxidative phosphorylation, biology.organism_classification, medicine.disease, Biochemistry, Cell biology, 03 medical and health sciences, 030104 developmental biology, Regulon, Membrane protein, Salmonella enterica, medicine, Protein folding, Molecular Biology

Abstract

The human pathogen Salmonella enterica serovar Typhimurium (S. Typhimurium) contains a complex disulfide bond (Dsb) catalytic machinery. This machinery encompasses multiple Dsb thiol-disulfide oxidoreductases that mediate oxidative protein folding and a less-characterized suppressor of copper sensitivity (scs) gene cluster, associated with increased tolerance to copper. To better understand the function of the Salmonella Scs system, here we characterized two of its key components, the membrane protein ScsB and the periplasmic protein ScsC. Our results revealed that these two proteins form a redox pair in which the electron transfer from the periplasmic domain of ScsB (n-ScsB) to ScsC is thermodynamically driven. We also demonstrate that the Scs reducing pathway remains separate from the Dsb oxidizing pathways and thereby avoids futile redox cycles. Additionally, we provide new insight into the molecular mechanism underlying Scs-mediated copper tolerance in Salmonella. We show that both ScsB and ScsC can bind toxic copper(I) with femtomolar affinities and transfer it to the periplasmic copper metallochaperone CueP. Our results indicate that the Salmonella Scs machinery has evolved a dual mode of action, capable of transferring reducing power to the oxidizing periplasm and protecting against copper stress by cooperating with the cue regulon, a major copper resistance mechanism in Salmonella. Overall, these findings expand our understanding of the functional diversity of Dsb-like systems, ranging from those mediating oxidative folding of proteins required for infection to those contributing to defense mechanisms against oxidative stress and copper toxicity, critical traits for niche adaptation and survival.

Published

2019

17. Structural bioinformatic analysis of DsbA proteins and their pathogenicity associated substrates

Author

Pramod Subedi, Geqing Wang, Jason J. Paxman, Makrina Totsika, Carlos F. Santos-Martin, Begoña Heras, and Lilian Hor

Subjects

Protein-protein interactions, Biophysics, Virulence, Computational biology, Review, Biochemistry, Protein–protein interaction, 03 medical and health sciences, Structural Biology, Oxidoreductase, Genetics, Protein secondary structure, 030304 developmental biology, ComputingMethodologies_COMPUTERGRAPHICS, chemistry.chemical_classification, 0303 health sciences, Disulfide bond, biology, Chemistry, Antimicrobials, Oxidative folding, 030302 biochemistry & molecular biology, biology.organism_classification, Thioredoxin proteins, 3. Good health, Computer Science Applications, DsbA, biology.protein, Protein folding, Bacteria, TP248.13-248.65, Biotechnology

Abstract

Graphical abstract, The disulfide bond (DSB) forming system and in particular DsbA, is a key bacterial oxidative folding catalyst. Due to its role in promoting the correct assembly of a wide range of virulence factors required at different stages of the infection process, DsbA is a master virulence rheostat, making it an attractive target for the development of new virulence blockers. Although DSB systems have been extensively studied across different bacterial species, to date, little is known about how DsbA oxidoreductases are able to recognize and interact with such a wide range of substrates. This review summarizes the current knowledge on the DsbA enzymes, with special attention on their interaction with the partner oxidase DsbB and substrates associated with bacterial virulence. The structurally and functionally diverse set of bacterial proteins that rely on DsbA-mediated disulfide bond formation are summarized. Local sequence and secondary structure elements of these substrates are analyzed to identify common elements recognized by DsbA enzymes. This not only provides information on protein folding systems in bacteria but also offers tools for identifying new DsbA substrates and informs current efforts aimed at developing DsbA targeted anti-microbials.

Published

2021

18. Fine tuning the mechanism of Antigen 43 self-association to modulate aggregation levels of Escherichia coli pathogens

Author

Julieanne L. Vo, Mark A. Schembri, Jason J. Paxman, Ageorges, Martínez Ortiz Gc, Begoña Heras, Alvin W. Lo, Mickaël Desvaux, Andrew E. Whitten, Nelly Caccia, Lilian Hor, Makrina Totsika, and Kate M. Peters

Subjects

biology, Chemistry, Mechanism (biology), Niche, Biofilm, biology.organism_classification, medicine.disease_cause, Cell biology, Antigen, Escherichia, medicine, Escherichia coli, Bacteria, Autotransporters

Abstract

Bacterial aggregates and biofilms allow bacteria to colonise a diverse array of surfaces that can ultimately lead to infections, where the protection they afford permits bacteria to resist anti-microbials and host immune factors. Despite these advantages there is a trade-off, whereby bacterial spread is reduced. As such, biofilm development needs to be regulated appropriately to suit the required niche. Here we investigate members from one of largest groups of bacterial adhesins, the autotransporters, for their critical role in the formation of bacterial aggregates and biofilms. We describe the structural and functional characterisation of autotransporter Ag43 homologues from diverse pathogenic Escherichia strains. We reveal a common mode of trans-association that leads to cell clumping and show that subtle variations in these interactions governs their aggregation kinetics. Our in depth investigation reveals an underlying molecular basis for the ‘tuning’ of bacterial aggregation.

Published

2021

19. Differential homotypic and heterotypic interactions of antigen 43 (Ag43) variants in autotransporter-mediated bacterial autoaggregation

Author

Grégory Jubelin, Begoña Heras, Ingrid Chafsey, Frédérique Chaucheyras-Durand, Xavier Bailly, Amanda E. Rossiter, Valentin Ageorges, Marion Schiavone, Ian R. Henderson, Mickaël Desvaux, Jason J. Paxman, Philippe Ruiz, Etienne Dague, Sabine Leroy, Nelly Caccia, Microbiologie Environnement Digestif Santé (MEDIS), Institut National de la Recherche Agronomique (INRA)-Université Clermont Auvergne [2017-2020] (UCA [2017-2020]), Lallemand SAS, Unité Mixte de Recherche d'Épidémiologie des maladies Animales et zoonotiques (UMR EPIA), Institut National de la Recherche Agronomique (INRA)-VetAgro Sup - Institut national d'enseignement supérieur et de recherche en alimentation, santé animale, sciences agronomiques et de l'environnement (VAS), Équipe Ingénierie pour les sciences du vivant (LAAS-ELIA), Laboratoire d'analyse et d'architecture des systèmes (LAAS), Université Toulouse Capitole (UT Capitole), Université de Toulouse (UT)-Université de Toulouse (UT)-Institut National des Sciences Appliquées - Toulouse (INSA Toulouse), Institut National des Sciences Appliquées (INSA)-Université de Toulouse (UT)-Institut National des Sciences Appliquées (INSA)-Université Toulouse - Jean Jaurès (UT2J), Université de Toulouse (UT)-Université Toulouse III - Paul Sabatier (UT3), Université de Toulouse (UT)-Centre National de la Recherche Scientifique (CNRS)-Institut National Polytechnique (Toulouse) (Toulouse INP), Université de Toulouse (UT)-Université Toulouse Capitole (UT Capitole), Université de Toulouse (UT), La Trobe University [Melbourne], Institute of Microbiology and Infection, University of Birmingham [Birmingham], INRA (Institut National de la Recherche Agronomique), CoMBa ('Colonisation de la Matrice extracellulaire Bacterienne') project - 'Region Auvergne' FRI ('Fond Regional Innovation') cluster IRP ('Institut de Recherche Pharmabiotique'), Australian Research Council (ARC) DP150102287 DP180102987 FT130100580, Conseil Regional d'Auvergne - FEDER (Fonds Europeen de Developpement Regional), INRA Clermont-Ferrand-Theix-Université Clermont Auvergne [2017-2020] (UCA [2017-2020]), Université Toulouse - Jean Jaurès (UT2J)-Université Toulouse 1 Capitole (UT1), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Institut National des Sciences Appliquées - Toulouse (INSA Toulouse), Institut National des Sciences Appliquées (INSA)-Institut National des Sciences Appliquées (INSA)-Institut National Polytechnique (Toulouse) (Toulouse INP), Université Fédérale Toulouse Midi-Pyrénées-Université Toulouse - Jean Jaurès (UT2J)-Université Toulouse 1 Capitole (UT1), Université Fédérale Toulouse Midi-Pyrénées, Microbiologie Environnement Digestif Santé - Clermont Auvergne (MEDIS), INRA Clermont-Ferrand-Theix-Université Clermont Auvergne (UCA), Unité de recherche d'Épidémiologie Animale (UEA), Institut National de la Recherche Agronomique (INRA), Institut National Polytechnique (Toulouse) (Toulouse INP), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Institut National des Sciences Appliquées - Toulouse (INSA Toulouse), Institut National des Sciences Appliquées (INSA)-Institut National des Sciences Appliquées (INSA)-Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Université Toulouse 1 Capitole (UT1)-Université Toulouse - Jean Jaurès (UT2J)-Institut National Polytechnique (Toulouse) (Toulouse INP), and Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Université Toulouse 1 Capitole (UT1)-Université Toulouse - Jean Jaurès (UT2J)

Subjects

0301 basic medicine, Signal peptide, Type V Secretion Systems, Molecular biology, [SDV]Life Sciences [q-bio], Structural alignment, lcsh:Medicine, Microbiology, Bacterial Adhesion, Article, spectroscopie, Bacterial genetics, sécrétion, 03 medical and health sciences, Bacterial secretion, 0302 clinical medicine, Phylogenetics, Secretion, lcsh:Science, Phylogeny, antigène, Adhesins, Escherichia coli, Antigens, Bacterial, Multidisciplinary, Chemistry, Escherichia coli Proteins, lcsh:R, Microbiology and Parasitology, Biological Transport, Antigenic Variation, Microbiologie et Parasitologie, Cell biology, Bacterial adhesin, 030104 developmental biology, Biofilms, lcsh:Q, escherichia coli, Bacterial outer membrane, 030217 neurology & neurosurgery, Bacterial Outer Membrane Proteins, Autotransporters

Abstract

Antigen 43 (Ag43) is a cell-surface exposed protein of Escherichia coli secreted by the Type V, subtype a, secretion system (T5aSS) and belonging to the family of self-associating autotransporters (SAATs). These modular proteins, comprising a cleavable N-terminal signal peptide, a surface-exposed central passenger and an outer membrane C-terminal translocator, self-recognise in a Velcro-like handshake mechanism. A phylogenetic network analysis focusing on the passenger revealed for the first time that they actually distribute into four distinct classes, namely C1, C2, C3 and C4. Structural alignment and modelling analyses demonstrated these classes arose from shuffling of two different subdomains within the Ag43 passengers. Functional analyses revealed that homotypic interactions occur for all Ag43 classes but significant differences in the sedimentation kinetics and aggregation state were present when Ag43C3 was expressed. In contrast, heterotypic interaction occurred in a very limited number of cases. Single cell-force spectroscopy demonstrated the importance of specific as well as nonspecific interactions in mediating Ag43-Ag43 recognition. We propose that structural differences in the subdomains of the Ag43 classes account for different autoaggregation dynamics and propensities to co-interact.

Published

2019

20. The Scs disulfide reductase system cooperates with the metallochaperone CueP in

Author

Pramod, Subedi, Jason J, Paxman, Geqing, Wang, Ashwinie A, Ukuwela, Zhiguang, Xiao, and Begoña, Heras

Subjects

Protein Folding, integumentary system, Adaptation, Physiological, Regulon, Metallochaperones, Bacterial Proteins, Salmonella, Drug Resistance, Bacterial, Periplasm, Enzymology, NADH, NADPH Oxidoreductases, Oxidation-Reduction, Copper, Protein Binding

Abstract

The human pathogen Salmonella enterica serovar Typhimurium (S. Typhimurium) contains a complex disulfide bond (Dsb) catalytic machinery. This machinery encompasses multiple Dsb thiol-disulfide oxidoreductases that mediate oxidative protein folding and a less-characterized suppressor of copper sensitivity (scs) gene cluster, associated with increased tolerance to copper. To better understand the function of the Salmonella Scs system, here we characterized two of its key components, the membrane protein ScsB and the periplasmic protein ScsC. Our results revealed that these two proteins form a redox pair in which the electron transfer from the periplasmic domain of ScsB (n-ScsB) to ScsC is thermodynamically driven. We also demonstrate that the Scs reducing pathway remains separate from the Dsb oxidizing pathways and thereby avoids futile redox cycles. Additionally, we provide new insight into the molecular mechanism underlying Scs-mediated copper tolerance in Salmonella. We show that both ScsB and ScsC can bind toxic copper(I) with femtomolar affinities and transfer it to the periplasmic copper metallochaperone CueP. Our results indicate that the Salmonella Scs machinery has evolved a dual mode of action, capable of transferring reducing power to the oxidizing periplasm and protecting against copper stress by cooperating with the cue regulon, a major copper resistance mechanism in Salmonella. Overall, these findings expand our understanding of the functional diversity of Dsb-like systems, ranging from those mediating oxidative folding of proteins required for infection to those contributing to defense mechanisms against oxidative stress and copper toxicity, critical traits for niche adaptation and survival.

Published

2019

21. Sortase-assembled pili promote extracellular electron transfer and iron acquisition inEnterococcus faecalisbiofilm

Author

Artur Matysik, Zhi Sheng Chua, Kimberly A. Kline, Jason J. Paxman, Begoña Heras, Jun Jie Wong, Kelvin Kian Long Chong, Pui Man Low, Ling Ning Lam, and Enrico Marsili

Subjects

Bacterial adhesin, biology, Sortase, Chemistry, Respiratory chain, Extracellular, Biofilm, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Enterococcus faecalis, Pilus, Bacteria, Microbiology

Abstract

Enterococcus faecalisis an opportunistic human pathogen and the cause of biofilm-associated infections of the heart, catheterized urinary tract, wounds, and the dysbiotic gut where it can expand to high numbers upon microbiome perturbations. TheE. faecalissortase-assembled endocarditis and biofilm associated pilus (Ebp) is involved in adhesion and biofilm formationin vitroandin vivo. Extracellular electron transfer (EET) also promotesE. faecalisbiofilm formation in iron-rich environments, however neither the mechanism underlying EET nor its role in virulence was previously known. Here we show that iron associated with Ebp serve as a terminal electron acceptor for EET, leading to extracellular iron reduction and intracellular iron accumulation. We found that a MIDAS motif within the EbpA tip adhesin is required for interaction with iron, EET, and FeoB-mediated iron uptake. We demonstrate that MenB and Ndh3, essential components of the aerobic respiratory chain and a specialized flavin-mediated electron transport chain, respectively, are required for iron-mediated EET. In addition, using a mouse gastrointestinal (GI) colonization model, we show that EET is essential for colonization of the GI tract, and Ebp is essential for augmentedE. faecalisGI colonization when dietary iron is in excess. Taken together, our findings show that pilus mediated capture of iron within biofilms enables EET-mediated iron acquisition inE. faecalis, and that these processes plays an important role inE. faecalisexpansion in the GI tract.SignificanceUnderstanding enterococcal biofilm development is the first step towards improved therapeutics for the often antimicrobial resistant infections caused by these bacteria. Here we report a role forEnterococcus faecalisendocarditis and biofilm associated pili (Ebp) in mediating iron-dependent biofilm growth and contributing to extracellular electron transfer (EET) which in turn promotes iron acquisition. Furthermore, we characterize the mechanisms underlying electron transfer in theE. faecalisbiofilm. Our findings support a model in whichE. faecalisuse EET to drive the reduction of pilus-associated ferric iron, leading to iron acquisition inE. faecalisbiofilm, and contributing to enterococcal virulence in the GI tract.

Published

2019

22. Structural Determinants Defining the Allosteric Inhibition of an Essential Antibiotic Target

Author

Jason J. Paxman, Tanzeela Siddiqui, Leanne M. Zammit, Natalia E. Ketaren, Nathan E. Hall, Matthew A. Perugini, Michael A. Gorman, Santosh Panjikar, Geoffrey B. Jameson, Belinda M. Abbott, Michael W. Parker, Tatiana P. Soares da Costa, Sebastien Desbois, Roy M. Robins-Browne, and Con Dogovski

Subjects

Models, Molecular, Protein Conformation, alpha-Helical, 0301 basic medicine, Dihydrodipicolinate synthase, Allosteric regulation, Lysine, Gene Expression, Biology, Crystallography, X-Ray, complex mixtures, Legionella pneumophila, Substrate Specificity, 03 medical and health sciences, Protein structure, Allosteric Regulation, Structural Biology, Escherichia coli, Protein Interaction Domains and Motifs, Amino Acid Sequence, Enzyme kinetics, Cloning, Molecular, Binding site, Molecular Biology, Hydro-Lyases, Feedback, Physiological, Binding Sites, Sequence Homology, Amino Acid, 030102 biochemistry & molecular biology, Microscale thermophoresis, Mutagenesis, Recombinant Proteins, Kinetics, Streptococcus pneumoniae, 030104 developmental biology, Biochemistry, biology.protein, bacteria, Protein Conformation, beta-Strand, Sequence Alignment, Allosteric Site, Protein Binding

Abstract

Dihydrodipicolinate synthase (DHDPS) catalyzes the first committed step in the lysine biosynthesis pathway of bacteria. The pathway can be regulated by feedback inhibition of DHDPS through the allosteric binding of the end product, lysine. The current dogma states that DHDPS from Gram-negative bacteria are inhibited by lysine but orthologs from Gram-positive species are not. The 1.65-Å resolution structure of the Gram-negative Legionella pneumophila DHDPS and the 1.88-Å resolution structure of the Gram-positive Streptococcus pneumoniae DHDPS bound to lysine, together with comprehensive functional analyses, show that this dogma is incorrect. We subsequently employed our crystallographic data with bioinformatics, mutagenesis, enzyme kinetics, and microscale thermophoresis to reveal that lysine-mediated inhibition is not defined by Gram staining, but by the presence of a His or Glu at position 56 (Escherichia coli numbering). This study has unveiled the molecular determinants defining lysine-mediated allosteric inhibition of bacterial DHDPS.

Published

2016

23. Structural and biochemical insights into the disulfide reductase mechanism of DsbD, an essential enzyme for neisserial pathogens

Author

Shakeel Mowlaboccus, Martin J. Scanlon, Roxanne P. Smith, Geqing Wang, Charlene M. Kahler, Begoña Heras, Martin Williams, Stephen J. Headey, Biswaranjan Mohanty, Pramod Subedi, Jason J. Paxman, and Bradley C. Doak

Subjects

0301 basic medicine, Models, Molecular, Protein Conformation, medicine.disease_cause, Crystallography, X-Ray, Biochemistry, 03 medical and health sciences, Protein structure, Bacterial Proteins, Protein Domains, Oxidoreductase, Catalytic Domain, medicine, Amino Acid Sequence, Disulfides, Molecular Biology, Escherichia coli, chemistry.chemical_classification, 030102 biochemistry & molecular biology, biology, Chemistry, Cell Biology, Periplasmic space, biology.organism_classification, Neisseria gonorrhoeae, 3. Good health, Transmembrane domain, 030104 developmental biology, Protein Structure and Folding, Protein folding, Neisseria, Oxidoreductases, Oxidation-Reduction

Abstract

The worldwide incidence of neisserial infections, particularly gonococcal infections, is increasingly associated with antibiotic-resistant strains. In particular, extensively drug-resistant Neisseria gonorrhoeae strains that are resistant to third-generation cephalosporins are a major public health concern. There is a pressing clinical need to identify new targets for the development of antibiotics effective against Neisseria-specific processes. In this study, we report that the bacterial disulfide reductase DsbD is highly prevalent and conserved among Neisseria spp. and that this enzyme is essential for survival of N. gonorrhoeae. DsbD is a membrane-bound protein that consists of two periplasmic domains, n-DsbD and c-DsbD, which flank the transmembrane domain t-DsbD. In this work, we show that the two functionally essential periplasmic domains of Neisseria DsbD catalyze electron transfer reactions through unidirectional interdomain interactions, from reduced c-DsbD to oxidized n-DsbD, and that this process is not dictated by their redox potentials. Structural characterization of the Neisseria n- and c-DsbD domains in both redox states provides evidence that steric hindrance reduces interactions between the two periplasmic domains when n-DsbD is reduced, thereby preventing a futile redox cycle. Finally, we propose a conserved mechanism of electron transfer for DsbD and define the residues involved in domain–domain recognition. Inhibitors of the interaction of the two DsbD domains have the potential to be developed as anti-neisserial agents.

Published

2018

24. NEW STRUCTURAL FEATURES REVEAL HOW BACTERIA STICK TO HOST SURFACES

Author

Alvin W. Lo, Chi Hao Luan, Santosh Panjikar, Jason J. Paxman, Begoña Heras, Mark A. Schembri, and Mike Kuiper

Subjects

Host (biology), Genetics, Biology, biology.organism_classification, Molecular Biology, Biochemistry, Bacteria, Biotechnology, Microbiology

Published

2018

25. Recognition by host nuclear transport proteins drives disorder-to-order transition in Hendra virus V

Author

Gregory W. Moseley, Natalie A. Borg, Sarah C. Atkinson, David A. Jans, Michelle D. Audsley, Ashley M. Buckle, Jason J. Paxman, Glenn A. Marsh, Kylie M. Wagstaff, Steven M. Heaton, Kim G. Lieu, and David R. Thomas

Subjects

Models, Molecular, 0301 basic medicine, Nucleocytoplasmic Transport Proteins, Immunoprecipitation, viruses, Molecular Conformation, lcsh:Medicine, Receptors, Cytoplasmic and Nuclear, Importin, Karyopherins, Intrinsically disordered proteins, Antiviral Agents, Article, Hendra Virus, Structure-Activity Relationship, Viral Proteins, 03 medical and health sciences, Drug Discovery, Humans, Protein Interaction Domains and Motifs, lcsh:Science, Cell Nucleus, Henipavirus Infections, Multidisciplinary, Chemistry, lcsh:R, virus diseases, Transporter, digestive system diseases, 3. Good health, Cell biology, Protein Transport, 030104 developmental biology, Interaction with host, Cytoplasm, Gene Knockdown Techniques, Host-Pathogen Interactions, lcsh:Q, Nuclear transport, Protein Binding

Abstract

Hendra virus (HeV) is a paramyxovirus that causes lethal disease in humans, for which no vaccine or antiviral agent is available. HeV V protein is central to pathogenesis through its ability to interact with cytoplasmic host proteins, playing key antiviral roles. Here we use immunoprecipitation, siRNA knockdown and confocal laser scanning microscopy to show that HeV V shuttles to and from the nucleus through specific host nuclear transporters. Spectroscopic and small angle X-ray scattering studies reveal HeV V undergoes a disorder-to-order transition upon binding to either importin α/β1 or exportin-1/Ran-GTP, dependent on the V N-terminus. Importantly, we show that specific inhibitors of nuclear transport prevent interaction with host transporters, and reduce HeV infection. These findings emphasize the critical role of host-virus interactions in HeV infection, and potential use of compounds targeting nuclear transport, such as the FDA-approved agent ivermectin, as anti-HeV agents.

Published

2018

26. Production, biophysical characterization and initial crystallization studies of the N- and C-terminal domains of DsbD, an essential enzyme in Neisseria meningitidis

Author

Martin J. Scanlon, Jason J. Paxman, Begoña Heras, Roxanne P. Smith, Charlene M. Kahler, and Andrew E. Whitten

Subjects

0301 basic medicine, Models, Molecular, Biophysics, Oxidative phosphorylation, Neisseria meningitidis, Crystallography, X-Ray, Biochemistry, Biophysical Phenomena, Research Communications, Electron Transport, 03 medical and health sciences, Bacterial Proteins, Protein Domains, X-Ray Diffraction, Structural Biology, Scattering, Small Angle, Genetics, Amino Acid Sequence, 030102 biochemistry & molecular biology, biology, Chemistry, Cytochrome c, Periplasmic space, Condensed Matter Physics, Recombinant Proteins, Transmembrane domain, 030104 developmental biology, Membrane protein, Cytoplasm, biology.protein, Protein folding, Thioredoxin, Crystallization, Oxidoreductases

Abstract

The membrane protein DsbD is a reductase that acts as an electron hub, translocating reducing equivalents from cytoplasmic thioredoxin to a number of periplasmic substrates involved in oxidative protein folding, cytochromecmaturation and oxidative stress defence. DsbD is a multi-domain protein consisting of a transmembrane domain (t-DsbD) flanked by two periplasmic domains (n-DsbD and c-DsbD). Previous studies have shown that DsbD is required for the survival of the obligate human pathogenNeisseria meningitidis. To help understand the structural and functional aspects ofN. meningitidisDsbD, the two periplasmic domains which are required for electron transfer are being studied. Here, the expression, purification and biophysical properties of n-NmDsbD and c-NmDsbD are described. The crystallization and crystallographic analysis of n-NmDsbD and c-NmDsbD are also described in both redox states, which differ only in the presence or absence of a disulfide bond but which crystallized in completely different conditions. Crystals of n-NmDsbDOx, n-NmDsbDRed, c-NmDsbDOxand c-NmDsbDReddiffracted to 2.3, 1.6, 2.3 and 1.7 Å resolution and belonged to space groupsP213,P321,P41andP1211, respectively.

Published

2018

27. The antigen 43 structure reveals a molecular Velcro-like mechanism of autotransporter-mediated bacterial clumping

Author

Matthew A. Perugini, Christine L. Gee, Mark A. Schembri, Begoña Heras, Kate M. Peters, Jason J. Paxman, Makrina Totsika, Andrew E. Whitten, and Russell Jarrott

Subjects

Plasma protein binding, Biology, Crystallography, X-Ray, medicine.disease_cause, Protein Structure, Secondary, Virulence factor, Microbiology, X-Ray Diffraction, medicine, Uropathogenic Escherichia coli, Cloning, Molecular, Adhesins, Bacterial, Mode of action, Escherichia coli, Adhesins, Escherichia coli, Antigens, Bacterial, Multidisciplinary, Biofilm, Biological Transport, Hydrogen Bonding, Biological Sciences, Cell aggregation, Protein Structure, Tertiary, Cell biology, Secretory protein, Structural biology, Biofilms, Mutation, Urinary Tract Infections, Protein Binding

Abstract

Aggregation and biofilm formation are critical mechanisms for bacterial resistance to host immune factors and antibiotics. Autotransporter (AT) proteins, which represent the largest group of outer-membrane and secreted proteins in Gram-negative bacteria, contribute significantly to these phenotypes. Despite their abundance and role in bacterial pathogenesis, most AT proteins have not been structurally characterized, and there is a paucity of detailed information with regard to their mode of action. Here we report the structure-function relationships of Antigen 43 (Ag43a), a prototypic self-associating AT protein from uropathogenic Escherichia coli. The functional domain of Ag43a displays a twisted L-shaped β-helical structure firmly stabilized by a 3D hydrogen-bonded scaffold. Notably, the distinctive Ag43a L shape facilitates self-association and cell aggregation. Combining all our data, we define a molecular "Velcro-like" mechanism of AT-mediated bacterial clumping, which can be tailored to fit different bacterial lifestyles such as the formation of biofilms.

Published

2013

28. Cloning to crystallization of dihydrodipicolinate synthase from the intracellular pathogenLegionella pneumophila

Author

Con Dogovski, Santosh Panjikar, Tanzeela Siddiqui, Matthew A. Perugini, and Jason J. Paxman

Subjects

Spectrometry, Mass, Electrospray Ionization, Dihydrodipicolinate synthase, Lysine, Intracellular Space, Biophysics, Crystallography, X-Ray, medicine.disease_cause, Biochemistry, Legionella pneumophila, law.invention, chemistry.chemical_compound, Biosynthesis, Structural Biology, law, Genetics, medicine, Molecular replacement, Cloning, Molecular, Crystallization, Escherichia coli, Hydro-Lyases, biology, bacterial infections and mycoses, Condensed Matter Physics, biology.organism_classification, Recombinant Proteins, respiratory tract diseases, chemistry, Crystallization Communications, biology.protein, bacteria, Electrophoresis, Polyacrylamide Gel, Protein quaternary structure

Abstract

Dihydrodipicolinate synthase (DHDPS) catalyses the rate-limiting step in the biosynthesis of meso-diaminopimelate and lysine. Here, the cloning, expression, purification and crystallization of DHDPS from the intracellular pathogen Legionella pneumophila are described. Crystals grown in the presence of high-molecular-weight PEG precipitant and magnesium chloride were found to diffract beyond 1.65 A resolution. The crystal lattice belonged to the hexagonal space group P6122, with unit-cell parameters a = b = 89.31, c = 290.18 A, and contained two molecules in the asymmetric unit. The crystal structure was determined by molecular replacement using a single chain of Pseudomonas aeruginosa DHDPS as the search model.

Published

2013

29. Bioinformatics Tools and Resources for Analyzing Protein Structures

Author

Jason J, Paxman and Begoña, Heras

Subjects

Models, Molecular, Structure-Activity Relationship, User-Computer Interface, Protein Conformation, Computational Biology, Proteins, Reproducibility of Results, Web Browser, Databases, Protein, Ligands, Software, Protein Binding

Abstract

The dramatic increase in the number of protein sequences and structures deposited in biological databases has led to the development of many bioinformatics tools and programs to manage, validate, compare, and interpret this large volume of data. In addition, powerful tools are being developed to use this sequence and structural data to facilitate protein classification and infer biological function of newly identified proteins. This chapter covers freely available bioinformatics resources on the World Wide Web that are commonly used for protein structure analysis.

Published

2016

30. Bioinformatics Tools and Resources for Analyzing Protein Structures

Author

Begoña Heras and Jason J. Paxman

Subjects

0301 basic medicine, 03 medical and health sciences, ComputingMethodologies_PATTERNRECOGNITION, 030104 developmental biology, Protein structure, 030102 biochemistry & molecular biology, Computer science, Protein structure analysis, Biological database, Computational biology, Bioinformatics, PDBsum, Function (biology)

Abstract

The dramatic increase in the number of protein sequences and structures deposited in biological databases has led to the development of many bioinformatics tools and programs to manage, validate, compare, and interpret this large volume of data. In addition, powerful tools are being developed to use this sequence and structural data to facilitate protein classification and infer biological function of newly identified proteins. This chapter covers freely available bioinformatics resources on the World Wide Web that are commonly used for protein structure analysis.

Published

2016

31. Targeting Bacterial Dsb Proteins for the Development of Anti-Virulence Agents

Author

Jason J. Paxman, Martin J. Scanlon, Begoña Heras, and Roxanne P. Smith

Subjects

Models, Molecular, 0301 basic medicine, Virulence Factors, medicine.drug_class, 030106 microbiology, Antibiotics, Quantitative Structure-Activity Relationship, Pharmaceutical Science, Virulence, Review, anti-virulence, DsbA inhibitors, Analytical Chemistry, Microbiology, lcsh:QD241-441, 03 medical and health sciences, Antibiotic resistance, Bacterial Proteins, lcsh:Organic chemistry, Drug Discovery, medicine, Humans, Computer Simulation, Physical and Theoretical Chemistry, fragment-based drug design, antimicrobial resistance, Uncategorized, Escherichia coli K12, biology, Drug discovery, Organic Chemistry, disulfide catalysis, Antimicrobial, biology.organism_classification, Anti-Bacterial Agents, High-Throughput Screening Assays, Multiple drug resistance, Oxidative Stress, 030104 developmental biology, DsbA, Chemistry (miscellaneous), biology.protein, Molecular Medicine, Bacteria, DsbB inhibitors

Abstract

Recent years have witnessed a dramatic increase in bacterial antimicrobial resistance and a decline in the development of novel antibiotics. New therapeutic strategies are urgently needed to combat the growing threat posed by multidrug resistant bacterial infections. The Dsb disulfide bond forming pathways are potential targets for the development of antimicrobial agents because they play a central role in bacterial pathogenesis. In particular, the DsbA/DsbB system catalyses disulfide bond formation in a wide array of virulence factors, which are essential for many pathogens to establish infections and cause disease. These redox enzymes are well placed as antimicrobial targets because they are taxonomically widespread, share low sequence identity with human proteins, and many years of basic research have provided a deep molecular understanding of these systems in bacteria. In this review, we discuss disulfide bond catalytic pathways in bacteria and their significance in pathogenesis. We also review the use of different approaches to develop inhibitors against Dsb proteins as potential anti-virulence agents, including fragment-based drug discovery, high-throughput screening and other structure-based drug discovery methods.

Published

2016

32. Front Cover: Autotransporter Adhesins in Escherichia coli Pathogenesis

Author

Begoña Heras, Shivakumar Keerthikumar, Jason J. Paxman, Suresh Mathivanan, Julieanne L. Vo, Gabriela Constanza Martínez Ortiz, and Pramod Subedi

Subjects

Bacterial adhesin, Pathogenesis, Front cover, medicine, Biology, medicine.disease_cause, Molecular Biology, Biochemistry, Escherichia coli, Microbiology

Published

2017

33. Autotransporter Adhesins in Escherichia coli Pathogenesis

Author

Julieanne L. Vo, Jason J. Paxman, Suresh Mathivanan, Gabriela Constanza Martínez Ortiz, Begoña Heras, Pramod Subedi, and Shivakumar Keerthikumar

Subjects

0301 basic medicine, Adhesins, Escherichia coli, 030106 microbiology, Gene Expression Regulation, Bacterial, Biology, biology.organism_classification, medicine.disease_cause, Biochemistry, Bacterial Adhesion, Microbiology, Bacterial adhesin, 03 medical and health sciences, Interaction with host, Escherichia coli, medicine, Autotransporter domain, Trimeric autotransporter adhesin, Bacterial outer membrane, Molecular Biology, Escherichia coli Infections, Bacteria, Biogenesis

Abstract

Most bacteria produce adhesion molecules to facilitate the interaction with host cells and establish successful infections. An important group of bacterial adhesins belong to the autotransporter (AT) superfamily, the largest group of secreted and outer membrane proteins in Gram-negative bacteria. AT adhesins possess diverse functions that facilitate bacterial colonisation, survival and persistence, and as such are often associated with increased bacterial fitness and pathogenic potential. In this review, we will describe AIDA-I type AT adhesins, which comprise the biggest and most diverse group in the AT family. We will focus on Escherichia coli proteins and define general aspects of their biogenesis, distribution, structural properties and key roles in infection.

Published

2017

34. Enzymology of Bacterial Lysine Biosynthesis

Author

Sudhir R. Dommaraju, Matthias Reumann, Lilian Hor, Con Dogovski, Nicole L. Taylor, Matthew T. Downton, Tanzeela Siddiqui, Theresa W. Qiu, Sarah C. Atkinson, Stephen Moore, Martin G. Peverelli, Jacinta M. Wubben, Jason J. Paxman, John Wagner, and Matthew A. Perugini

Subjects

chemistry.chemical_classification, biology, fungi, Lysine, biology.organism_classification, complex mixtures, carbohydrates (lipids), Cell wall, chemistry.chemical_compound, chemistry, Biochemistry, Protein biosynthesis, bacteria, Moiety, Peptidoglycan, Lysine biosynthesis, Essential amino acid, Bacteria

Abstract

Lysine is an essential amino acid in the mammalian diet, but can be synthesised de novo in bacteria, plants and some fungi (Dogovski et al., 2009; Hutton et al., 2007). In bacteria, the lysine biosynthesis pathway, also known as the diaminopimelate (DAP) pathway (Fig. 1), yields the important metabolites meso-2,6-diaminopimelate (meso-DAP) and lysine. Lysine is utilised for protein synthesis in bacteria and forms part of the peptidoglycan cross-link structure in the cell wall of most Gram-positive species; whilst meso-DAP is the peptidoglycan cross-linking moiety in the cell wall of Gram-negative bacteria and also Gram-positive Bacillus species (Burgess et al., 2008; Mitsakos et al., 2008; Voss et al., 2010) (Fig. 1).

Published

2012

35. The Structure of the Bacterial Oxidoreductase Enzyme DsbA in Complex with a Peptide Reveals a Basis for Substrate Specificity in the Catalytic Cycle of DsbA Enzymes

Author

Philip E. Thompson, Natalie A. Borg, Martin J. Scanlon, Stephen P. Bottomley, Charlene M. Kahler, Jamie Rossjohn, Mary Catherine Pearce, Harry Sakellaris, Yanni K.-Y. Chin, Pooja Sharma, Susannah Piek, Jamie S. Simpson, James Horne, Jason J. Paxman, and Jerome Wielens

Subjects

Models, Molecular, Magnetic Resonance Spectroscopy, Protein Conformation, Molecular Sequence Data, Protein Disulfide-Isomerases, Crystallography, X-Ray, Biochemistry, Catalysis, Substrate Specificity, Bacterial Proteins, Oxidoreductase, Escherichia coli, Amino Acid Sequence, Disulfides, Binding site, Molecular Biology, chemistry.chemical_classification, Binding Sites, biology, Sequence Homology, Amino Acid, Escherichia coli Proteins, Active site, Membrane Proteins, Cell Biology, Peptide Fragments, DsbA, chemistry, Catalytic cycle, Protein Structure and Folding, biology.protein, Protein folding, Domain of unknown function, Thioredoxin

Abstract

Oxidative protein folding in Gram-negative bacteria results in the formation of disulfide bonds between pairs of cysteine residues. This is a multistep process in which the dithiol-disulfide oxidoreductase enzyme, DsbA, plays a central role. The structure of DsbA comprises an all helical domain of unknown function and a thioredoxin domain, where active site cysteines shuttle between an oxidized, substrate-bound, reduced form and a DsbB-bound form, where DsbB is a membrane protein that reoxidizes DsbA. Most DsbA enzymes interact with a wide variety of reduced substrates and show little specificity. However, a number of DsbA enzymes have now been identified that have narrow substrate repertoires and appear to interact specifically with a smaller number of substrates. The transient nature of the DsbA-substrate complex has hampered our understanding of the factors that govern the interaction of DsbA enzymes with their substrates. Here we report the crystal structure of a complex between Escherichia coli DsbA and a peptide with a sequence derived from a substrate. The binding site identified in the DsbA-peptide complex was distinct from that observed for DsbB in the DsbA-DsbB complex. The structure revealed details of the DsbA-peptide interaction and suggested a mechanism by which DsbA can simultaneously show broad specificity for substrates yet exhibit specificity for DsbB. This mode of binding was supported by solution nuclear magnetic resonance data as well as functional data, which demonstrated that the substrate specificity of DsbA could be modified via changes at the binding interface identified in the structure of the complex.

36. Antigen 43 associated with Escherichia coli membrane vesicles contributes to bacterial cell association and biofilm formation.

Author

Zavan L, Hor L, Johnston EL, Paxman J, Heras B, and Kaparakis-Liaskos M

Abstract

Bacterial membrane vesicles (MVs) are produced by all bacteria and contribute to numerous bacterial functions due to their ability to package and transfer bacterial cargo. In doing so, MVs have been shown to facilitate horizontal gene transfer, mediate antimicrobial activity, and promote biofilm formation. Uropathogenic Escherichia coli is a pathogenic Gram-negative organism that persists in the urinary tract of its host due to its ability to form persistent, antibiotic-resistant biofilms. The formation of these biofilms is dependent upon proteins such as Antigen 43 (Ag43), which belongs to the widespread Autotransporter group of bacterial surface proteins. In E. coli, the autotransporter Ag43 has been shown to contribute to bacterial cell aggregation and biofilm formation via self-association of Ag43 between neighboring Ag43-expressing bacteria. As MVs package bacterial proteins, we investigated whether MVs produced by E. coli contained Ag43, and the ability of Ag43-expressing MVs to facilitate cell aggregation and biofilm formation. We showed that Ag43 expressing E. coli produced MVs that contained Ag43 on their surface and had an enhanced ability to bind to E. coli bacteria. Furthermore, we demonstrated that the addition of Ag43-containing MVs to Ag43-expressing E. coli significantly enhanced biofilm formation. These findings reveal the contribution of MVs harboring autotransporters in promoting bacterial aggregation and enhancing biofilm formation, highlighting the impact of MVs and their specific composition to bacterial adaptation and pathogenesis.IMPORTANCEAutotransporter proteins are the largest family of outer membrane and secreted proteins in Gram-negative bacteria which contribute to pathogenesis by promoting aggregation, biofilm formation, persistence, and cytotoxicity. Although the roles of bacterial autotransporters are well known, the ability of bacterial membrane vesicles (MVs) naturally released from the surface of bacteria to contain autotransporters and their role in promoting virulence remains less investigated. Our findings reveal that MVs produced by E. coli contain the autotransporter protein Ag43. Furthermore, we show that Ag43-containing MVs function to enhance bacterial cell interactions and biofilm formation. By demonstrating the ability of MVs to carry functional autotransporter adhesins, this work highlights the importance of MVs in disseminating autotransporters beyond the bacterial cell membrane to ultimately promote cellular interactions and enhance biofilm development. Overall, these findings have significant implications in furthering our understanding of the numerous ways in which MVs can facilitate bacterial persistence and pathogenesis.

Published

2025

37. Stereotactic Vertebroplasty for Spinal Metastases with Multilevel Bilateral Pedicle Fractures: A Technical Note.

Author

Ziu M, Traylor JI, Paxman J, and Goodgame BW

Abstract

Vertebral compression fractures (VCFs) represent a significant cause of disability and primarily result from either underlying vertebral body neoplasms or osteoporosis. Vertebroplasty (VP) is a procedure commonly utilized to repair pathologic VCFs in order to manage pain and reinstate vertebral body height. However, there is a paucity of literature on how to manage painful multilevel VCFs with concomitant bilateral pedicle fractures. We describe a patient with a primary prostatic carcinoma and VCFs of the third and fourth lumbar vertebrae (L3 and L4, respectively) with concomitant bilateral pedicle fractures secondary to metastatic disease. Due to the degree of damage to the L3 and L4 vertebral bodies and pedicles, a VP performed via a percutaneous approach was deemed to be too high risk. VP for L3 and L4 was instead performed by utilizing stereotactic spine navigation and an intraoperative O-arm (Medtronic Corporation, Minneapolis, Minnesota). Our result indicates a potential role for stereotactic spine navigation in vertebroplasty for complex pathologic VCFs., Competing Interests: The authors have declared that no competing interests exist.

Published

2019

38. Utilizing Stereotactic Spine Navigation for Posterior Partial Vertebrectomy in an En Bloc Resection of a Superior Pulmonary Sulcus Tumor Invading the Thoracic Vertebrae: A Technical Note.

Author

Ziu M, Traylor JI, Paxman J, Gorrebeeck A, and Fortes DL

Abstract

Prior to the development of en bloc techniques, vertebral invasion by non-small cell lung cancer (NSCLC) had been considered a relative contraindication to surgical intervention. However, reports in the literature have demonstrated increased progression-free survival with the use of neoadjuvant chemotherapy followed by anterior en bloc resection of the residual tumor. Stereotactic spine navigation has been shown to improve accuracy during complex vertebral osteotomies, improving patient outcomes. We report a 53-year-old woman with an NSCLC in the left upper lobe, a periosteum attachment of the second and third thoracic vertebrae (T2 and T3, respectively), and an infiltration of the corresponding nerve roots. We describe a surgical approach for the resection of NSCLC with vertebral infiltration utilizing stereotactic spine navigation and intraoperative computed tomography (CT) (O-Arm, Medtronic, Minneapolis, Minnesota, US) for a posterior approach laminectomy, osteotomy, and partial vertebrectomy, followed by trans-thoracic en bloc resection of a superior pulmonary sulcus tumor with nerve root infiltration. Posterior approach vertebral osteotomy and en bloc resection for superior sulcus NSCLC infiltrating the vertebrae utilizing stereotactic spine navigation and intraoperative CT (O-Arm) is a viable alternative to the traditional anterior approach., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

39. Drunken Membranes: Short-Chain Alcohols Alter Fusion of Liposomes to Planar Lipid Bilayers.

Author

Paxman J, Hunt B, Hallan D, Zarbock SR, and Woodbury DJ

Subjects

Dose-Response Relationship, Drug, Exocytosis drug effects, Membrane Fluidity drug effects, Ethanol chemistry, Ethanol pharmacology, Lipid Bilayers metabolism, Liposomes metabolism, Membrane Fusion drug effects

Abstract

Although the effects of ethanol on protein receptors and lipid membranes have been studied extensively, ethanol's effect on vesicles fusing to lipid bilayers is not known. To determine the effect of alcohols on fusion rates, we utilized the nystatin/ergosterol fusion assay to measure fusion of liposomes to a planar lipid bilayer (BLM). The addition of ethanol excited fusion when applied on the cis (vesicle) side, and inhibited fusion on the trans side. Other short-chain alcohols followed a similar pattern. In general, the inhibitory effect of alcohols (trans) occurs at lower doses than the excitatory (cis) effect, with a decrease of 29% in fusion rates at the legal driving limit of 0.08% (w/v) ethanol (IC 50  = 0.2% v/v, 34 mM). Similar inhibitory effects were observed with methanol, propanol, and butanol, with ethanol being the most potent. Significant variability was observed with different alcohols when applied to the cis side. Ethanol and propanol enhanced fusion, butanol also enhanced fusion but was less potent, and low doses of methanol mildly inhibited fusion. The inhibition by trans addition of alcohols implies that they alter the planar membrane structure and thereby increase the activation energy required for fusion, likely through an increase in membrane fluidity. The cis data are likely a combination of the above effect and a proportionally greater lowering of the vesicle lysis tension and hydration repulsive pressure that combine to enhance fusion. Alternate hypotheses are also discussed. The inhibitory effect of ethanol on liposome-membrane fusion is large enough to provide a possible biophysical explanation of compromised neuronal behavior., (Copyright © 2017 Biophysical Society. Published by Elsevier Inc. All rights reserved.)

Published

2017